病原微生物综合分析云平台

Basic Information

Accession number

GCA_001040825.1

Release date

2015-06-26

Organism

Salmonella enterica subsp. enterica serovar Derby

Species name

Salmonella enterica

Assembly level

Scaffold

Assembly name

ASM104082v1

Assembly submitter

ANSES

Assembly Type

haploid

Genome size

4.8 Mb

GC percent

52.0

Contig count

Collection date

2007

Sample location

France: Brittany

Host

pig

Isolation source

Isolate type

Strain

07CR553

Isolate

ARG List

ORF_ID	Pass_Bitscore	Best_Hit_Bitscore	Best_Hit_ARO	Best_Identities	ARO	Model_type	SNPs_in_Best_Hit_ARO	Drug class	Resistance mechanism	AMR gene family	Description
LAZB01000013.1_11 # 6753 # 7952	700.0	768.459	tet(A)	98.48	ARO:3000165	protein homolog model		tetracycline antibiotic	antibiotic efflux	major facilitator superfamily (MFS) antibiotic efflux pump	TetA is a tetracycline efflux pump found in many species of Gram-negative bacteria.
LAZB01000002.1_28 # 24865 # 26322	940.0	963.37	mdsC	98.97	ARO:3000791	protein homolog model		monobactam; carbapenem; cephalosporin; cephamycin; penam; phenicol antibiotic; penem	antibiotic efflux	resistance-nodulation-cell division (RND) antibiotic efflux pump	MdsC is the outer membrane channel of the multidrug and metal efflux complex MdsABC.
LAZB01000002.1_29 # 26339 # 29506	2090.0	2113.58	mdsB	99.62	ARO:3000790	protein homolog model		monobactam; carbapenem; cephalosporin; cephamycin; penam; phenicol antibiotic; penem	antibiotic efflux	resistance-nodulation-cell division (RND) antibiotic efflux pump	MdsB is the inner membrane transporter of the multidrug and metal efflux complex MdsABC. mdsB corresponds to 1 locus in Pseudomonas aeruginosa PAO1 (gene name: mexQ) and 2 loci in Pseudomonas aeruginosa LESB58.
LAZB01000002.1_30 # 29503 # 30729	770.0	810.061	mdsA	99.26	ARO:3000789	protein homolog model		monobactam; carbapenem; cephalosporin; cephamycin; penam; phenicol antibiotic; penem	antibiotic efflux	resistance-nodulation-cell division (RND) antibiotic efflux pump	MdsA is the membrane fusion protein of the multidrug and metal efflux complex MdsABC.
LAZB01000002.1_32 # 33306 # 33770	290.0	319.316	golS	100.0	ARO:3000504	protein homolog model		monobactam; carbapenem; cephalosporin; cephamycin; penam; phenicol antibiotic; penem	antibiotic efflux	resistance-nodulation-cell division (RND) antibiotic efflux pump	GolS is a regulator activated by the presence of golD, and promotes the expression of the MdsABC efflux pump.
LAZB01000002.1_58 # 65997 # 67109	250.0	268.47	vanG	38.98	ARO:3002909	protein homolog model		glycopeptide antibiotic	antibiotic target alteration	glycopeptide resistance gene cluster; Van ligase	VanG is a D-Ala-D-Ala ligase homolog that can synthesize D-Ala-D-Ser, an alternative substrate for peptidoglycan synthesis that reduces vancomycin binding affinity in Enterococcus faecalis.
LAZB01000002.1_149 # 160400 # 163549	1900.0	2001.87	acrB	94.57	ARO:3000216	protein homolog model		fluoroquinolone antibiotic; cephalosporin; glycylcycline; penam; tetracycline antibiotic; rifamycin antibiotic; phenicol antibiotic; disinfecting agents and antiseptics	antibiotic efflux	resistance-nodulation-cell division (RND) antibiotic efflux pump	Protein subunit of AcrA-AcrB-TolC multidrug efflux complex. AcrB functions as a herterotrimer which forms the inner membrane component and is primarily responsible for substrate recognition and energy transduction by acting as a drug/proton antiporter.
LAZB01000002.1_150 # 163572 # 164765	670.0	696.812	Escherichia coli acrA	91.94	ARO:3004043	protein homolog model		fluoroquinolone antibiotic; cephalosporin; glycylcycline; penam; tetracycline antibiotic; rifamycin antibiotic; phenicol antibiotic; disinfecting agents and antiseptics	antibiotic efflux	resistance-nodulation-cell division (RND) antibiotic efflux pump	AcrA is a subunit of the AcrAB-TolC multidrug efflux system found in E. coli.
LAZB01000018.1_17 # 17298 # 17975	400.0	426.402	kdpE	92.41	ARO:3003841	protein homolog model		aminoglycoside antibiotic	antibiotic efflux	kdpDE	kdpE is a transcriptional activator that is part of the two-component system KdpD/KdpE that is studied for its regulatory role in potassium transport and has been identified as an adaptive regulator involved in the virulence and intracellular survival of pathogenic bacteria. kdpE regulates a range of virulence loci through direct promoter binding.
LAZB01000019.1_77 # 74925 # 75455	280.0	337.806	emrR	93.14	ARO:3000516	protein homolog model		fluoroquinolone antibiotic	antibiotic efflux	major facilitator superfamily (MFS) antibiotic efflux pump	EmrR is a negative regulator for the EmrAB-TolC multidrug efflux pump in E. coli. Mutations lead to EmrAB-TolC overexpression.
LAZB01000019.1_78 # 75582 # 76754	675.0	706.057	emrA	89.74	ARO:3000027	protein homolog model		fluoroquinolone antibiotic	antibiotic efflux	major facilitator superfamily (MFS) antibiotic efflux pump	EmrA is a membrane fusion protein, providing an efflux pathway with EmrB and TolC between the inner and outer membranes of E. coli, a Gram-negative bacterium.
LAZB01000019.1_79 # 76771 # 78309	900.0	996.882	emrB	95.7	ARO:3000074	protein homolog model		fluoroquinolone antibiotic	antibiotic efflux	major facilitator superfamily (MFS) antibiotic efflux pump	emrB is a translocase in the emrB -TolC efflux protein in E. coli. It recognizes substrates including carbonyl cyanide m-chlorophenylhydrazone (CCCP), nalidixic acid, and thioloactomycin.
LAZB01000019.1_85 # 84344 # 84529	100.0	109.383	rsmA	85.25	ARO:3005069	protein homolog model		fluoroquinolone antibiotic; diaminopyrimidine antibiotic; phenicol antibiotic	antibiotic efflux	resistance-nodulation-cell division (RND) antibiotic efflux pump	rsmA is a gene that regulates virulence of Pseudomonas aeruginosa. However, its negative effect on MexEF-OprN overexpression has been noted to confer resistance to various antibiotics. It's Escherichia coli homolog is csrA.
LAZB01000003.1_19 # 20081 # 23194	1900.0	2016.12	acrD	94.21	ARO:3000491	protein homolog model		aminoglycoside antibiotic	antibiotic efflux	resistance-nodulation-cell division (RND) antibiotic efflux pump	AcrD is an aminoglycoside efflux pump expressed in E. coli. Its expression can be induced by indole, and is regulated by baeRS and cpxAR.
LAZB01000027.1_49 # 53309 # 54148	500.0	553.132	sul1	100.0	ARO:3000410	protein homolog model		sulfonamide antibiotic	antibiotic target replacement	sulfonamide resistant sul	Sul1 is a sulfonamide resistant dihydropteroate synthase of Gram-negative bacteria. It is linked to other resistance genes of class 1 integrons.
LAZB01000027.1_50 # 54142 # 54489	190.0	219.55	qacEdelta1	100.0	ARO:3005010	protein homolog model		disinfecting agents and antiseptics	antibiotic efflux	major facilitator superfamily (MFS) antibiotic efflux pump	QacEdelta1 is a resistance gene conferring resistance to antiseptics. It is different from QacE only at the 3'-terminus.
LAZB01000027.1_51 # 54653 # 55432	450.0	522.316	aadA2	100.0	ARO:3002602	protein homolog model		aminoglycoside antibiotic	antibiotic inactivation	ANT(3'')	aadA2 is an aminoglycoside nucleotidyltransferase gene encoded by plasmids and integrons in K. pneumoniae, Salmonella spp., Corynebacterium glutamicum, C. freundii and Aeromonas spp.
LAZB01000004.1_69 # 67381 # 68754	890.0	908.286	cpxA	96.94	ARO:3000830	protein homolog model		aminoglycoside antibiotic; aminocoumarin antibiotic	antibiotic efflux	resistance-nodulation-cell division (RND) antibiotic efflux pump	CpxA is a membrane-localized sensor kinase that is activated by envelope stress. It starts a kinase cascade that activates CpxR, which promotes efflux complex expression.
LAZB01000029.1_126 # 144130 # 145074	500.0	583.178	leuO	86.94	ARO:3003843	protein homolog model		nucleoside antibiotic; disinfecting agents and antiseptics	antibiotic efflux	major facilitator superfamily (MFS) antibiotic efflux pump	leuO, a LysR family transcription factor, exists in a wide variety of bacteria of the family Enterobacteriaceae and is involved in the regulation of as yet unidentified genes affecting the stress response and pathogenesis expression. LeuO is also an activator of the MdtNOP efflux pump.
LAZB01000029.1_312 # 353905 # 355146	700.0	705.286	mdtM	85.78	ARO:3001214	protein homolog model		fluoroquinolone antibiotic; lincosamide antibiotic; nucleoside antibiotic; phenicol antibiotic; disinfecting agents and antiseptics	antibiotic efflux	major facilitator superfamily (MFS) antibiotic efflux pump	Multidrug resistance protein MdtM.
LAZB01000029.1_334 # 376230 # 376652	250.0	284.648	FosA7	96.43	ARO:3004113	protein homolog model		phosphonic acid antibiotic	antibiotic inactivation	fosfomycin thiol transferase	FosA7 is an enzyme that confers resistance to fosfomycin in Escherichia coli by breaking the epoxide ring of the molecule.
LAZB01000005.1_184 # 188681 # 189403	470.0	499.59	sdiA	98.75	ARO:3000826	protein homolog model		fluoroquinolone antibiotic; cephalosporin; glycylcycline; penam; tetracycline antibiotic; rifamycin antibiotic; phenicol antibiotic; disinfecting agents and antiseptics	antibiotic efflux	resistance-nodulation-cell division (RND) antibiotic efflux pump	SdiA is a cell division regulator that is also a positive regulator of AcrAB only when it's expressed from a plasmid. When the sdiA gene is on the chromosome, it has no effect on expression of acrAB.
LAZB01000005.1_365 # 376763 # 378511	1000.0	1160.59	msbA	96.39	ARO:3003950	protein homolog model		nitroimidazole antibiotic	antibiotic efflux	ATP-binding cassette (ABC) antibiotic efflux pump	MsbA is a multidrug resistance transporter homolog from E. coli and belongs to a superfamily of transporters that contain an adenosine triphosphate (ATP) binding cassette (ABC) which is also called a nucleotide-binding domain (NBD). MsbA is a member of the MDR-ABC transporter group by sequence homology. MsbA transports lipid A, a major component of the bacterial outer cell membrane, and is the only bacterial ABC transporter that is essential for cell viability.
LAZB01000005.1_439 # 464466 # 465698	700.0	726.087	Escherichia coli mdfA	87.93	ARO:3001328	protein homolog model		tetracycline antibiotic; disinfecting agents and antiseptics	antibiotic efflux	major facilitator superfamily (MFS) antibiotic efflux pump	Multidrug efflux pump in E. coli. This multidrug efflux system was originally identified as the Cmr/CmlA chloramphenicol exporter.
LAZB01000005.1_619 # 659379 # 659816	275.0	301.212	AAC(6')-Iy	97.93	ARO:3002569	protein homolog model		aminoglycoside antibiotic	antibiotic inactivation	AAC(6')	AAC(6')-Iy is a chromosomal-encoded aminoglycoside acetyltransferase in S. enteritidis and S. enterica. Regulatory mutation required to increase expression of this chromosomally-encoded gene for resistance. In the specific system, aminoglycoside resistance was due to a transcriptional fusion secondary to a chromosomal deletion in which the downstream aac(6')-Iy gene was placed under the control of the upstream nmpC promoter.
LAZB01000005.1_733 # 779811 # 780194	230.0	251.136	marA	95.24	ARO:3000263	protein homolog model		fluoroquinolone antibiotic; monobactam; carbapenem; cephalosporin; glycylcycline; cephamycin; penam; tetracycline antibiotic; rifamycin antibiotic; phenicol antibiotic; penem; disinfecting agents and antiseptics	antibiotic efflux; reduced permeability to antibiotic	resistance-nodulation-cell division (RND) antibiotic efflux pump; General Bacterial Porin with reduced permeability to beta-lactams	In the presence of antibiotic stress, E. coli overexpresses the global activator protein MarA, which besides inducing MDR efflux pump AcrAB, also down- regulates synthesis of the porin OmpF.
LAZB01000005.1_771 # 816314 # 816643	150.0	185.267	Klebsiella pneumoniae KpnF	87.16	ARO:3004583	protein homolog model		macrolide antibiotic; aminoglycoside antibiotic; cephalosporin; tetracycline antibiotic; peptide antibiotic; rifamycin antibiotic; disinfecting agents and antiseptics	antibiotic efflux	small multidrug resistance (SMR) antibiotic efflux pump	KpnF subunit of KpnEF resembles EbrAB from E. coli. Mutation in KpnEF resulted in increased susceptibility to cefepime, ceftriaxon, colistin, erythromycin, rifampin, tetracycline, and streptomycin as well as enhanced sensitivity toward sodium dodecyl sulfate, deoxycholate, dyes, benzalkonium chloride, chlorhexidine, and triclosan.
LAZB01000005.1_772 # 816630 # 816992	150.0	177.178	Klebsiella pneumoniae KpnE	76.67	ARO:3004580	protein homolog model		macrolide antibiotic; aminoglycoside antibiotic; cephalosporin; tetracycline antibiotic; peptide antibiotic; rifamycin antibiotic; disinfecting agents and antiseptics	antibiotic efflux	small multidrug resistance (SMR) antibiotic efflux pump	KpnE subunit of KpnEF resembles EbrAB from E. coli. Mutation in KpnEF resulted in increased susceptibility to cefepime, ceftriaxon, colistin, erythromycin, rifampin, tetracycline, and streptomycin as well as enhanced sensitivity toward sodium dodecyl sulfate, deoxycholate, dyes, benzalkonium chloride, chlorhexidine, and triclosan.
LAZB01000005.1_1167 # 1206140 # 1207564	900.0	927.546	MdtK	99.37	ARO:3001327	protein homolog model		fluoroquinolone antibiotic	antibiotic efflux	multidrug and toxic compound extrusion (MATE) transporter	A multidrug and toxic compound extrusions (MATE) transporter conferring resistance to norfloxacin, doxorubicin and acriflavine.
LAZB01000005.1_1240 # 1275059 # 1276225	700.0	716.072	ugd	89.18	ARO:3003577	protein homolog model		peptide antibiotic	antibiotic target alteration	pmr phosphoethanolamine transferase	PmrE is required for the synthesis and transfer of 4-amino-4-deoxy-L-arabinose (Ara4N) to Lipid A, which allows gram-negative bacteria to resist the antimicrobial activity of cationic antimicrobial peptides and antibiotics such as polymyxin.
LAZB01000005.1_1288 # 1332596 # 1335718	1800.0	1873.21	mdtB	91.83	ARO:3000793	protein homolog model		aminocoumarin antibiotic	antibiotic efflux	resistance-nodulation-cell division (RND) antibiotic efflux pump	MdtB is a transporter that forms a heteromultimer complex with MdtC to form a multidrug transporter. MdtBC is part of the MdtABC-TolC efflux complex.
LAZB01000005.1_1289 # 1335719 # 1338799	1800.0	1861.27	mdtC	91.61	ARO:3000794	protein homolog model		aminocoumarin antibiotic	antibiotic efflux	resistance-nodulation-cell division (RND) antibiotic efflux pump	MdtC is a transporter that forms a heteromultimer complex with MdtB to form a multidrug transporter. MdtBC is part of the MdtABC-TolC efflux complex. In the absence of MdtB, MdtC can form a homomultimer complex that results in a functioning efflux complex with a narrower drug specificity. mdtC corresponds to 3 loci in Pseudomonas aeruginosa PAO1 (gene name: muxC/muxB) and 3 loci in Pseudomonas aeruginosa LESB58.
LAZB01000005.1_1292 # 1341608 # 1342330	450.0	469.544	baeR	96.67	ARO:3000828	protein homolog model		aminoglycoside antibiotic; aminocoumarin antibiotic	antibiotic efflux	resistance-nodulation-cell division (RND) antibiotic efflux pump	BaeR is a response regulator that promotes the expression of MdtABC and AcrD efflux complexes.
LAZB01000006.1_22 # 16415 # 17047	400.0	432.95	CRP	99.05	ARO:3000518	protein homolog model		macrolide antibiotic; fluoroquinolone antibiotic; penam	antibiotic efflux	resistance-nodulation-cell division (RND) antibiotic efflux pump	CRP is a global regulator that represses MdtEF multidrug efflux pump expression.
LAZB01000008.1_45 # 51986 # 52969	550.0	589.341	PmrF	87.42	ARO:3003578	protein homolog model		peptide antibiotic	antibiotic target alteration	pmr phosphoethanolamine transferase	PmrF is required for the synthesis and transfer of 4-amino-4-deoxy-L-arabinose (Ara4N) to Lipid A, which allows gram-negative bacteria to resist the antimicrobial activity of cationic antimicrobial peptides and antibiotics such as polymyxin. pmrF corresponds to 1 locus in Pseudomonas aeruginosa PAO1 and 1 locus in Pseudomonas aeruginosa LESB58.
LAZB01000008.1_48 # 55841 # 57487	400.0	710.679	ArnT	62.43	ARO:3005053	protein homolog model		peptide antibiotic	antibiotic target alteration	pmr phosphoethanolamine transferase	ArnT is involved in Cell Wall Biosynthesis, specifically 4-amino-4-deoxy-L-arabinose (Ara4N). It confers resistance to peptide antibiotics.
LAZB01000008.1_283 # 312336 # 313160	500.0	528.865	bacA	96.72	ARO:3002986	protein homolog model		peptide antibiotic	antibiotic target alteration	undecaprenyl pyrophosphate related proteins	The bacA gene product (BacA) recycles undecaprenyl pyrophosphate during cell wall biosynthesis which confers resistance to bacitracin.
LAZB01000015.1_29 # 27803 # 29194	850.0	905.205	Escherichia coli UhpT with mutation conferring resistance to fosfomycin	95.46	ARO:3003890	protein variant model	E350Q	phosphonic acid antibiotic	antibiotic target alteration	antibiotic-resistant UhpT	Mutations to the active importer UhpT, which is involved with the uptake of many phosphorylated sugars, confer resistance to fosfomycin by reducing import of the drug into the bacteria.
LAZB01000016.1_47 # 26212 # 27396	700.0	796.579	Escherichia coli EF-Tu mutants conferring resistance to Pulvomycin	99.49	ARO:3003369	protein variant model	R234F	elfamycin antibiotic	antibiotic target alteration	elfamycin resistant EF-Tu	Sequence variants of Escherichia coli elongation factor Tu that confer resistance to Pulvomycin.
LAZB01000029.1_119 # 136151 # 137917	500.0	587.8	Haemophilus influenzae PBP3 conferring resistance to beta-lactam antibiotics	52.9	ARO:3004446	protein variant model	D350N, S357N	cephalosporin; cephamycin; penam	antibiotic target alteration	Penicillin-binding protein mutations conferring resistance to beta-lactam antibiotics	PBP3 is a penicillin-binding protein and beta-lactam resistance enzyme encoded by the ftsI gene in Haemophilus influenzae. Mutations in ftsI confer resistance to beta-lactam antibiotics.
LAZB01000008.1_30 # 35354 # 36712	850.0	895.575	Escherichia coli GlpT with mutation conferring resistance to fosfomycin	96.9	ARO:3003889	protein variant model	E448K	phosphonic acid antibiotic	antibiotic target alteration	antibiotic-resistant GlpT	Point mutations to the active importer GlpT, which is involved with the uptake of many phosphorylated sugars, confer resistance to fosfomycin by reducing import of the drug into the bacteria.
LAZB01000002.1_151 # 164907 # 165560	375.0	395.201	Escherichia coli AcrAB-TolC with AcrR mutation conferring resistance to ciprofloxacin, tetracycline, and ceftazidime	87.38	ARO:3003807	protein overexpression model		fluoroquinolone antibiotic; cephalosporin; glycylcycline; penam; tetracycline antibiotic; rifamycin antibiotic; phenicol antibiotic; disinfecting agents and antiseptics	antibiotic target alteration; antibiotic efflux	resistance-nodulation-cell division (RND) antibiotic efflux pump	AcrR is a repressor of the AcrAB-TolC multidrug efflux complex. AcrR mutations result in high level antibiotic resistance. The mutations associated with this model are specific to E. coli.
LAZB01000029.1_585 # 646272 # 646730	300.0	300.056	Escherichia coli soxR with mutation conferring antibiotic resistance	96.05	ARO:3003381	protein overexpression model		fluoroquinolone antibiotic; cephalosporin; glycylcycline; penam; tetracycline antibiotic; rifamycin antibiotic; phenicol antibiotic; disinfecting agents and antiseptics	antibiotic target alteration; antibiotic efflux	ATP-binding cassette (ABC) antibiotic efflux pump; major facilitator superfamily (MFS) antibiotic efflux pump; resistance-nodulation-cell division (RND) antibiotic efflux pump	SoxR is a sensory protein that upregulates soxS expression in the presence of redox-cycling drugs. This stress response leads to the expression many multidrug efflux pumps.
LAZB01000029.1_586 # 646817 # 647140	200.0	212.231	Escherichia coli soxS with mutation conferring antibiotic resistance	95.33	ARO:3003511	protein overexpression model		fluoroquinolone antibiotic; monobactam; carbapenem; cephalosporin; glycylcycline; cephamycin; penam; tetracycline antibiotic; rifamycin antibiotic; phenicol antibiotic; penem; disinfecting agents and antiseptics	antibiotic target alteration; antibiotic efflux; reduced permeability to antibiotic	ATP-binding cassette (ABC) antibiotic efflux pump; major facilitator superfamily (MFS) antibiotic efflux pump; resistance-nodulation-cell division (RND) antibiotic efflux pump; General Bacterial Porin with reduced permeability to beta-lactams	SoxS is a global regulator that up-regulates the expression of AcrAB efflux genes. It also reduces OmpF expression to decrease cell membrane permeability.
LAZB01000005.1_732 # 779357 # 779791	210.0	273.478	Escherichia coli AcrAB-TolC with MarR mutations conferring resistance to ciprofloxacin and tetracycline	92.36	ARO:3003378	protein overexpression model		fluoroquinolone antibiotic; cephalosporin; glycylcycline; penam; tetracycline antibiotic; rifamycin antibiotic; phenicol antibiotic; disinfecting agents and antiseptics	antibiotic target alteration; antibiotic efflux	resistance-nodulation-cell division (RND) antibiotic efflux pump	MarR is a repressor of the mar operon marRAB, thus regulating the expression of marA, the activator of multidrug efflux pump AcrAB.

VF List

Query_id	%Identity	E-value	Related genes	VF ID	Virulence factor	VFcategory	VFcategoryID	Characteristics	Description	Strain
LAZB01000010.1_4	67.897	1.25E-127	IlpA	VF0513	IlpA	Adherence	VFC0001		(IlpA) immunogenic lipoprotein A [IlpA (VF0513) - Adherence (VFC0001)] [Vibrio vulnificus YJ016]	Vibrio vulnificus
LAZB01000011.1_29	98.928	0.0	bapA	VF0971	BapA	Adherence	VFC0001	"
LAZB01000012.1_63	64.881	2.72E-168	rffG	VF0044	LOS	Immune modulation	VFC0258	Lic1A (phosphorylcholine (ChoP) kinase) 5'-CAAT-3' within the 5'-end of its coding sequence; lic2A, also referred to as lexA, variation in the number of 5'-CAAT-3' repeats has been shown to correlate directly with phase variation of the Gal-alpha(1-4)beta-Gal LPS structure; But lgtC (glycosyltransferase), another phase-variable gene, ultimately dictates whether this structure is synthesized. lic3A encode a sialyl transferase which directs the substitution of LPS with sialic acid.	(rffG) dTDP-glucose 46-dehydratase [LOS (VF0044) - Immune modulation (VFC0258)] [Haemophilus influenzae Rd KW20]	Haemophilus influenzae
LAZB01000015.1_45	99.559	2.7E-167	mgtC	VF1365	MgtC	Nutritional/Metabolic factor	VFC0272	An inner membrane protein; anti-virulence protein CigR inhibits the virulence functions of MgtC at early times inside macrophages	(mgtC) Salmonella virulence protein MgtC [MgtC (VF1365) - Nutritional/Metabolic factor (VFC0272)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000015.1_46	99.67	0.0	mgtB	VF0106	MgtB	Nutritional/Metabolic factor	VFC0272	A magnesium transporter	(mgtB) Mg2+ transport protein [MgtB (VF0106) - Nutritional/Metabolic factor (VFC0272)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000015.1_52	98.534	0.0	misL	VF0397	MisL	Adherence	VFC0001	MisL is located within Salmonella Pathogenicity Island SPI-3	(misL) putative autotransporter [MisL (VF0397) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000015.1_101	63.714	1.96E-157	rfaF	VF0044	LOS	Immune modulation	VFC0258	Lic1A (phosphorylcholine (ChoP) kinase) 5'-CAAT-3' within the 5'-end of its coding sequence; lic2A, also referred to as lexA, variation in the number of 5'-CAAT-3' repeats has been shown to correlate directly with phase variation of the Gal-alpha(1-4)beta-Gal LPS structure; But lgtC (glycosyltransferase), another phase-variable gene, ultimately dictates whether this structure is synthesized. lic3A encode a sialyl transferase which directs the substitution of LPS with sialic acid.	(rfaF) ADP-heptose-LPS heptosyltransferase II [LOS (VF0044) - Immune modulation (VFC0258)] [Haemophilus influenzae Rd KW20]	Haemophilus influenzae
LAZB01000015.1_102	77.922	0.0	rfaD	VF0044	LOS	Immune modulation	VFC0258	Lic1A (phosphorylcholine (ChoP) kinase) 5'-CAAT-3' within the 5'-end of its coding sequence; lic2A, also referred to as lexA, variation in the number of 5'-CAAT-3' repeats has been shown to correlate directly with phase variation of the Gal-alpha(1-4)beta-Gal LPS structure; But lgtC (glycosyltransferase), another phase-variable gene, ultimately dictates whether this structure is synthesized. lic3A encode a sialyl transferase which directs the substitution of LPS with sialic acid.	(rfaD) ADP-L-glycero-D-mannoheptose-6-epimerase [LOS (VF0044) - Immune modulation (VFC0258)] [Haemophilus influenzae Rd KW20]	Haemophilus influenzae
LAZB01000016.1_47	80.153	0.0	tufA	VF0460	EF-Tu	Adherence	VFC0001		(tufA) elongation factor Tu [EF-Tu (VF0460) - Adherence (VFC0001)] [Francisella tularensis subsp. tularensis SCHU S4]	Francisella tularensis
LAZB01000002.1_29	60.383	0.0	adeG	VF0504	AdeFGH efflux pump	Biofilm	VFC0271	Belongs to resistance-nodulation-cell division (RND)-type efflux system; RND efflux systems, composed of an inner membrane protein (RND pump) linked by a periplasmic adaptor protein (PAP) to an outer membrane factor (OMF), can extrude a wide range of substrates often unrelated in structure; To date, three Acinetobacter drug efflux (Ade) RND systems, AdeABC, AdeFGH, and AdeIJK, have been characterized in A. baumannii	(adeG) cation/multidrug efflux pump [AdeFGH efflux pump (VF0504) - Biofilm (VFC0271)] [Acinetobacter baumannii ACICU]	Acinetobacter baumannii
LAZB01000002.1_124	66.495	2.42E-98	clpP	VF0074	ClpP	Stress survival	VFC0282	21.6 kDa protein belongs to a family of proteases highly conserved in prokaryotes and eukaryotes	(clpP) ATP-dependent Clp protease proteolytic subunit [ClpP (VF0074) - Stress survival (VFC0282)] [Listeria monocytogenes EGD-e]	Listeria monocytogenes
LAZB01000002.1_149	92.088	0.0	acrB	VF0568	AcrAB	Antimicrobial activity/Competitive advantage	VFC0325		(acrB) acriflavine resistance protein B [AcrAB (VF0568) - Antimicrobial activity/Competitive advantage (VFC0325)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000002.1_150	85.279	0.0	acrA	VF0568	AcrAB	Antimicrobial activity/Competitive advantage	VFC0325		(acrA) acriflavine resistance protein A [AcrAB (VF0568) - Antimicrobial activity/Competitive advantage (VFC0325)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000002.1_188	73.77	4.84E-172	allS	VF0572	Allantion utilization	Nutritional/Metabolic factor	VFC0272	An allantoin utilization operon has been associated with hypervirulent K. pneumoniae strains that cause pyogenic liver abscesses.	(allS) DNA-binding transcriptional activator AllS [Allantion utilization (VF0572) - Nutritional/Metabolic factor (VFC0272)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000002.1_189	78.75	1.05E-94	allA	VF0572	Allantion utilization	Nutritional/Metabolic factor	VFC0272	An allantoin utilization operon has been associated with hypervirulent K. pneumoniae strains that cause pyogenic liver abscesses.	(allA) ureidoglycolate hydrolase [Allantion utilization (VF0572) - Nutritional/Metabolic factor (VFC0272)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000002.1_190	85.874	9.99E-177	allR	VF0572	Allantion utilization	Nutritional/Metabolic factor	VFC0272	An allantoin utilization operon has been associated with hypervirulent K. pneumoniae strains that cause pyogenic liver abscesses.	(allR) DNA-binding transcriptional repressor AllR [Allantion utilization (VF0572) - Nutritional/Metabolic factor (VFC0272)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000002.1_196	93.377	0.0	allB	VF0572	Allantion utilization	Nutritional/Metabolic factor	VFC0272	An allantoin utilization operon has been associated with hypervirulent K. pneumoniae strains that cause pyogenic liver abscesses.	(allB) allantoinase [Allantion utilization (VF0572) - Nutritional/Metabolic factor (VFC0272)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000002.1_200	80.44	0.0	allC	VF0572	Allantion utilization	Nutritional/Metabolic factor	VFC0272	An allantoin utilization operon has been associated with hypervirulent K. pneumoniae strains that cause pyogenic liver abscesses.	(allC) allantoate amidohydrolase [Allantion utilization (VF0572) - Nutritional/Metabolic factor (VFC0272)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000002.1_201	81.662	0.0	allD	VF0572	Allantion utilization	Nutritional/Metabolic factor	VFC0272	An allantoin utilization operon has been associated with hypervirulent K. pneumoniae strains that cause pyogenic liver abscesses.	(allD) ureidoglycolate dehydrogenase [Allantion utilization (VF0572) - Nutritional/Metabolic factor (VFC0272)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000002.1_216	97.838	3.57E-131	fimA	VF0102	Type 1 fimbriae	Adherence	VFC0001	Chaperone-usher assembly pathway	(fimA) type-1 fimbrial protein subunit A [Type 1 fimbriae (VF0102) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000002.1_217	98.305	5.28E-130	fimI	VF0102	Type 1 fimbriae	Adherence	VFC0001	Chaperone-usher assembly pathway	(fimI) fimbrial protein internal segment [Type 1 fimbriae (VF0102) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000002.1_218	98.261	3.74E-168	fimC	VF0102	Type 1 fimbriae	Adherence	VFC0001	Chaperone-usher assembly pathway	(fimC) chaperone protein FimC [Type 1 fimbriae (VF0102) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000002.1_219	98.966	0.0	fimD	VF0102	Type 1 fimbriae	Adherence	VFC0001	Chaperone-usher assembly pathway	(fimD) usher protein FimD [Type 1 fimbriae (VF0102) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000002.1_220	99.701	0.0	fimH	VF0102	Type 1 fimbriae	Adherence	VFC0001	Chaperone-usher assembly pathway	(fimH) type I fimbriae minor fimbrial subunit FimH, adhesin [Type 1 fimbriae (VF0102) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000002.1_221	99.419	7.33E-126	fimF	VF0102	Type 1 fimbriae	Adherence	VFC0001	Chaperone-usher assembly pathway	(fimF) type I fimbriae adaptor protein FimF [Type 1 fimbriae (VF0102) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000002.1_222	100.0	1.07E-155	fimZ	VF0102	Type 1 fimbriae	Adherence	VFC0001	Chaperone-usher assembly pathway	(fimZ) DNA-binding response regulator [Type 1 fimbriae (VF0102) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000002.1_223	97.5	2.95E-175	fimY	VF0102	Type 1 fimbriae	Adherence	VFC0001	Chaperone-usher assembly pathway	(fimY) fimbriae Y protein [Type 1 fimbriae (VF0102) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000002.1_225	99.495	3.93E-149	fimW	VF0102	Type 1 fimbriae	Adherence	VFC0001	Chaperone-usher assembly pathway	(fimW) helix-turn-helix transcriptional regulator [Type 1 fimbriae (VF0102) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000002.1_230	88.889	0.0	gtrB	VF0124	LPS	Immune modulation	VFC0258	Composed of the O-antigen, core polysaccharides and lipid A; the genes involved in the biosynthesis of the basic O-antigen are located in the rfb/rfc loci; O-antigen modification is associated with temperate bacteriophages. Four different serotype-converting phages have been found: SfII, Sf6, SfV and SfX, which are involved in conversion of a serotype Y stain to serotypes 2a, 3b, 5a and X, respectively	(gtrB) bactoprenol glucosyl transferase [LPS (VF0124) - Immune modulation (VFC0258)] [Shigella flexneri 2a str. 301]	Shigella flexneri
LAZB01000002.1_231	80.0	1.26E-70	gtrA	VF0124	LPS	Immune modulation	VFC0258	Composed of the O-antigen, core polysaccharides and lipid A; the genes involved in the biosynthesis of the basic O-antigen are located in the rfb/rfc loci; O-antigen modification is associated with temperate bacteriophages. Four different serotype-converting phages have been found: SfII, Sf6, SfV and SfX, which are involved in conversion of a serotype Y stain to serotypes 2a, 3b, 5a and X, respectively	(gtrA) bactoprenol-linked glucose translocase/flippase [LPS (VF0124) - Immune modulation (VFC0258)] [Shigella flexneri 2a str. 301]	Shigella flexneri
LAZB01000002.1_257	81.987	0.0	fepA	VF0228	Enterobactin	Nutritional/Metabolic factor	VFC0272	An extremely effective iron chelator, with a formation constant for the iron complex of 1049. Fe3+ is coordinated by six catechol oxygens to form a metal chelate with a net negative charge of three	(fepA) ferrienterobactin outer membrane transporter [Enterobactin (VF0228) - Nutritional/Metabolic factor (VFC0272)] [Escherichia coli CFT073]	Escherichia coli (UPEC)
LAZB01000002.1_258	74.372	0.0	fes	VF0228	Enterobactin	Nutritional/Metabolic factor	VFC0272	An extremely effective iron chelator, with a formation constant for the iron complex of 1049. Fe3+ is coordinated by six catechol oxygens to form a metal chelate with a net negative charge of three	(fes) enterobactin/ferric enterobactin esterase [Enterobactin (VF0228) - Nutritional/Metabolic factor (VFC0272)] [Escherichia coli CFT073]	Escherichia coli (UPEC)
LAZB01000002.1_260	79.289	0.0	entF	VF0228	Enterobactin	Nutritional/Metabolic factor	VFC0272	An extremely effective iron chelator, with a formation constant for the iron complex of 1049. Fe3+ is coordinated by six catechol oxygens to form a metal chelate with a net negative charge of three	(entF) enterobactin synthase multienzyme complex component, ATP-dependent [Enterobactin (VF0228) - Nutritional/Metabolic factor (VFC0272)] [Escherichia coli CFT073]	Escherichia coli (UPEC)
LAZB01000002.1_261	72.654	0.0	fepE	VF0228	Enterobactin	Nutritional/Metabolic factor	VFC0272	An extremely effective iron chelator, with a formation constant for the iron complex of 1049. Fe3+ is coordinated by six catechol oxygens to form a metal chelate with a net negative charge of three	(fepE) LPS O-antigen length regulator [Enterobactin (VF0228) - Nutritional/Metabolic factor (VFC0272)] [Escherichia coli CFT073]	Escherichia coli (UPEC)
LAZB01000002.1_262	92.015	0.0	fepC	VF0228	Enterobactin	Nutritional/Metabolic factor	VFC0272	An extremely effective iron chelator, with a formation constant for the iron complex of 1049. Fe3+ is coordinated by six catechol oxygens to form a metal chelate with a net negative charge of three	(fepC) ferrienterobactin ABC transporter ATPase [Enterobactin (VF0228) - Nutritional/Metabolic factor (VFC0272)] [Escherichia coli CFT073]	Escherichia coli (UPEC)
LAZB01000002.1_263	86.93	0.0	fepG	VF0228	Enterobactin	Nutritional/Metabolic factor	VFC0272	An extremely effective iron chelator, with a formation constant for the iron complex of 1049. Fe3+ is coordinated by six catechol oxygens to form a metal chelate with a net negative charge of three	(fepG) iron-enterobactin ABC transporter permease [Enterobactin (VF0228) - Nutritional/Metabolic factor (VFC0272)] [Escherichia coli CFT073]	Escherichia coli (UPEC)
LAZB01000002.1_264	84.478	0.0	fepD	VF0562	Ent	Nutritional/Metabolic factor	VFC0272	Various iron acquisition systems in Klebsiella are needed to overcome host defenses in different anatomical compartments.	(fepD) iron-enterobactin transporter membrane protein [Ent (VF0562) - Nutritional/Metabolic factor (VFC0272)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000002.1_265	90.465	0.0	entS	VF0228	Enterobactin	Nutritional/Metabolic factor	VFC0272	An extremely effective iron chelator, with a formation constant for the iron complex of 1049. Fe3+ is coordinated by six catechol oxygens to form a metal chelate with a net negative charge of three	(entS) enterobactin exporter, iron-regulated [Enterobactin (VF0228) - Nutritional/Metabolic factor (VFC0272)] [Escherichia coli CFT073]	Escherichia coli (UPEC)
LAZB01000002.1_266	79.56	0.0	fepB	VF0228	Enterobactin	Nutritional/Metabolic factor	VFC0272	An extremely effective iron chelator, with a formation constant for the iron complex of 1049. Fe3+ is coordinated by six catechol oxygens to form a metal chelate with a net negative charge of three	(fepB) ferrienterobactin ABC transporter periplasmic binding protein [Enterobactin (VF0228) - Nutritional/Metabolic factor (VFC0272)] [Escherichia coli CFT073]	Escherichia coli (UPEC)
LAZB01000002.1_267	84.143	0.0	entC	VF0228	Enterobactin	Nutritional/Metabolic factor	VFC0272	An extremely effective iron chelator, with a formation constant for the iron complex of 1049. Fe3+ is coordinated by six catechol oxygens to form a metal chelate with a net negative charge of three	(entC) isochorismate synthase 1 [Enterobactin (VF0228) - Nutritional/Metabolic factor (VFC0272)] [Escherichia coli CFT073]	Escherichia coli (UPEC)
LAZB01000002.1_268	86.142	0.0	entE	VF0228	Enterobactin	Nutritional/Metabolic factor	VFC0272	An extremely effective iron chelator, with a formation constant for the iron complex of 1049. Fe3+ is coordinated by six catechol oxygens to form a metal chelate with a net negative charge of three	(entE) 2,3-dihydroxybenzoate-AMP ligase component of enterobactin synthase multienzyme complex [Enterobactin (VF0228) - Nutritional/Metabolic factor (VFC0272)] [Escherichia coli CFT073]	Escherichia coli (UPEC)
LAZB01000002.1_269	88.07	0.0	entB	VF0228	Enterobactin	Nutritional/Metabolic factor	VFC0272	An extremely effective iron chelator, with a formation constant for the iron complex of 1049. Fe3+ is coordinated by six catechol oxygens to form a metal chelate with a net negative charge of three	(entB) isochorismatase [Enterobactin (VF0228) - Nutritional/Metabolic factor (VFC0272)] [Escherichia coli CFT073]	Escherichia coli (UPEC)
LAZB01000002.1_270	89.516	1.9E-164	entA	VF0228	Enterobactin	Nutritional/Metabolic factor	VFC0272	An extremely effective iron chelator, with a formation constant for the iron complex of 1049. Fe3+ is coordinated by six catechol oxygens to form a metal chelate with a net negative charge of three	(entA) 2,3-dihydro-2,3-dihydroxybenzoate dehydrogenase EntA [Enterobactin (VF0228) - Nutritional/Metabolic factor (VFC0272)] [Escherichia coli CFT073]	Escherichia coli (UPEC)
LAZB01000018.1_7	100.0	4.99E-111	fur	VF0113	Fur	Regulation	VFC0301		(fur) ferric iron uptake transcriptional regulator [Fur (VF0113) - Regulation (VFC0301)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000018.1_29	62.703	2.76E-79	fimB	VF0566	Type I fimbriae	Adherence	VFC0001	Type I fimbriae are expressed in 90% of both clinical and environmental K. pneumoniae isolates as well as almost all members of the Enterobacteriaceae.; Type I fimbriae are filamentous, membrane-bound, adhesive structures composed primarily of FimA subunits, with the FimH subunit on the tip.	(fimB) tyrosine recombinase [Type I fimbriae (VF0566) - Adherence (VFC0001)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000018.1_32	76.501	0.0	rfbD	VF0561	LPS	Immune modulation	VFC0258	In K. pneumoniae there are nine main O-serotypes. Three of these, O1, O2, and O3, are responsible for almost 80% of all Klebsiella infections.; Compared with other Enterobacteriaceae, such as Escherichia coli 161 defined O serotypes and Shigella flexneri at least 47 O serotypes, Klebsiella has a surprisingly low number of reported O serotypes which promises a more viable alternative for vaccine development compared with K-antigen-based vaccines; The O-antigen biosynthesis enzymes are encoded on the rfb locus.	(rfbD) UDP-galactopyranose mutase [LPS (VF0561) - Immune modulation (VFC0258)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000018.1_34	69.6	0.0	KP1_RS17225	VF0561	LPS	Immune modulation	VFC0258	In K. pneumoniae there are nine main O-serotypes. Three of these, O1, O2, and O3, are responsible for almost 80% of all Klebsiella infections.; Compared with other Enterobacteriaceae, such as Escherichia coli 161 defined O serotypes and Shigella flexneri at least 47 O serotypes, Klebsiella has a surprisingly low number of reported O serotypes which promises a more viable alternative for vaccine development compared with K-antigen-based vaccines; The O-antigen biosynthesis enzymes are encoded on the rfb locus.	(KP1_RS17225) glycosyltransferase family 4 protein [LPS (VF0561) - Immune modulation (VFC0258)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000019.1_35	86.523	0.0	iroB	VF0230	Salmochelin siderophore	Nutritional/Metabolic factor	VFC0272	Also identified as virulence factors in extracellular pathogenic Escherichia coli and Salmonella enterica serotype Typhi	(iroB) glucosyltransferase IroB [Salmochelin siderophore (VF0230) - Nutritional/Metabolic factor (VFC0272)] [Escherichia coli CFT073]	Escherichia coli (UPEC)
LAZB01000019.1_36	81.803	0.0	iroC	VF0563	Sal	Nutritional/Metabolic factor	VFC0272	Salmochelin is a glycosylated Ent that requires the iroA locus for production and transport	(iroC) ABC transporter [Sal (VF0563) - Nutritional/Metabolic factor (VFC0272)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000019.1_37	68.608	0.0	iroD	VF0230	Salmochelin siderophore	Nutritional/Metabolic factor	VFC0272	Also identified as virulence factors in extracellular pathogenic Escherichia coli and Salmonella enterica serotype Typhi	(iroD) esterase [Salmochelin siderophore (VF0230) - Nutritional/Metabolic factor (VFC0272)] [Escherichia coli CFT073]	Escherichia coli (UPEC)
LAZB01000019.1_38	61.27	2.46E-129	iroE	VF0230	Salmochelin siderophore	Nutritional/Metabolic factor	VFC0272	Also identified as virulence factors in extracellular pathogenic Escherichia coli and Salmonella enterica serotype Typhi	(iroE) esterase [Salmochelin siderophore (VF0230) - Nutritional/Metabolic factor (VFC0272)] [Escherichia coli CFT073]	Escherichia coli (UPEC)
LAZB01000019.1_39	83.84	0.0	iroN	VF0563	Sal	Nutritional/Metabolic factor	VFC0272	Salmochelin is a glycosylated Ent that requires the iroA locus for production and transport	(iroN) salmochelin receptor IroN [Sal (VF0563) - Nutritional/Metabolic factor (VFC0272)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000019.1_41	88.286	0.0	pipB2	VF0947	TTSS-2 secreted effectors	Effector delivery system	VFC0086		(pipB2) type III secretion system effector PipB3 [TTSS-2 secreted effectors (VF0947) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_43	95.638	0.0	mig-14	VF0395	Mig-14	Antimicrobial activity/Competitive advantage	VFC0325	Mig-14 expression is induced within macrophages and is under the control of the global regulator PhoP	(mig-14) antimicrobial peptide resistance protein Mig-14 [Mig-14 (VF0395) - Antimicrobial activity/Competitive advantage (VFC0325)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_81	71.93	2.39E-93	luxS	VF0406	AI-2	Biofilm	VFC0271	AI-2 is produced and detected by a wide variety of bacteria and is presumed to facilitate interspecies communications.	(luxS) S-ribosylhomocysteinase [AI-2 (VF0406) - Biofilm (VFC0271)] [Vibrio cholerae O1 biovar El Tor str. N16961]	Vibrio cholerae
LAZB01000019.1_85	76.667	1.4E-30	csrA	VF0261	CsrA	Regulation	VFC0301	Belongs to a highly conserved family of global regulators that typically control stationary phase traits post-transcriptionally	(csrA) carbon storage regulator CsrA [CsrA (VF0261) - Regulation (VFC0301)] [Legionella pneumophila subsp. pneumophila str. Philadelphia 1]	Legionella pneumophila
LAZB01000019.1_125	99.306	0.0	avrA	VF0949	TTSS-1 secreted effectors	Effector delivery system	VFC0086		(avrA) type III secretion system effector AvrA, acetyltransferease [TTSS-1 secreted effectors (VF0949) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_126	98.406	0.0	sprB	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(sprB) transcriptional regulator [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_127	99.661	0.0	hilC	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(hilC) AraC family transcriptional regulator [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_128	97.333	1.81E-107	orgC	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(orgC) type III secretion system effector OrgC [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_129	100.0	1.82E-169	orgB/SctL	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(orgB/SctL) type III secretion system stator OrgB [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_130	98.958	1.87E-139	orgA/sctK	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(orgA/sctK) type III secretion system accessory cytosolic protein OrgA [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_131	100.0	0.0	prgK	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(prgK) type III secretion system inner MS ring protein PrgK [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_132	100.0	4.28E-70	prgJ	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(prgJ) type III secretion system inner rod protein PrgJ [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_133	96.25	3.35E-53	prgI	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(prgI) type III secretion system needle filament protein PrgI [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_134	99.49	0.0	prgH	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(prgH) type III secretion system outer MS ring protein PrgH [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_135	100.0	0.0	hilD	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(hilD) AraC family transcriptional regulator [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_136	100.0	0.0	hilA	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(hilA) transcriptional regulator [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_137	98.75	1.15E-118	iagB	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(iagB) invasion protein IagB [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_138	97.196	0.0	sptP	VF0949	TTSS-1 secreted effectors	Effector delivery system	VFC0086		(sptP) type III secretion system effector SptP, tyrosine phosphatase and GTPase-activating protein [TTSS-1 secreted effectors (VF0949) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_139	98.462	3.59E-92	sicP	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(sicP) chaparone for SptP [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_141	98.78	4.73E-55	iacP	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(iacP) putative acyl carrier protein [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_142	97.81	0.0	sipA/sspA	VF0949	TTSS-1 secreted effectors	Effector delivery system	VFC0086		(sipA/sspA) type III secretion system effector SipA (Salmonella invasion protein A) [TTSS-1 secreted effectors (VF0949) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_143	99.417	0.0	sipD	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(sipD) type III secretion system hydrophilic translocator, needle tip protein SipD [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_144	99.756	0.0	sipC/sspC	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(sipC/sspC) type III secretion system hydrophilic translocator, pore protein SipC [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_145	99.831	0.0	sipB/sspB	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(sipB/sspB) type III secretion system hydrophilic translocator, pore protein SipB (Salmonella invasion protein B) [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_146	100.0	1.17E-124	sicA	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(sicA) chaparone for SipC and SipB [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_147	100.0	0.0	spaS	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(spaS) type III secretion system export apparatus switch protein SpaS [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_148	100.0	0.0	spaR	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(spaR) type III secretion system minor export apparatus protein SpaR [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_149	100.0	1.03E-56	spaQ	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(spaQ) type III secretion system minor export apparatus protein SpaQ [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_150	100.0	1.06E-165	spaP	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(spaP) type III secretion system minor export apparatus protein SpaP [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_151	100.0	0.0	spaO/sctQ	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(spaO/sctQ) type III secretion system C ring protein SpaO [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_152	99.107	0.0	invJ	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(invJ) type III secretion system needle length regulator InvJ [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_153	99.32	2.44E-99	invI	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(invI) type III secretion system stalk protein InvI [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_154	100.0	0.0	invC/sctN	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(invC/sctN) type III secretion system ATPase InvC [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_155	100.0	5.36E-99	invB	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(invB) type III secretion system protein InvB [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_156	100.0	0.0	invA	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(invA) type III secretion system major export apparatus protein InvA [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_157	99.731	0.0	invE	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(invE) type III secretion system gatekeeper invE [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_158	99.822	0.0	invG	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(invG) type III secretion system secretin invG [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_159	99.537	1.11E-162	invF	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(invF) type III secretion system regulatory protein InvF [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_160	99.32	2.83E-106	invH	VF0116	TTSS (SPI-1 encode)	Effector delivery system	VFC0086		(invH) type III secretion system pilotin invG [TTSS (SPI-1 encode) (VF0116) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_180	100.0	0.0	rpoS	VF0112	RpoS	Regulation	VFC0301		(rpoS) RNA polymerase sigma factor RpoS [RpoS (VF0112) - Regulation (VFC0301)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000019.1_201	99.054	0.0	sopD	VF0949	TTSS-1 secreted effectors	Effector delivery system	VFC0086		(sopD) type III secretion system effector SopD [TTSS-1 secreted effectors (VF0949) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000021.1_12	99.715	0.0	STM0266	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_13	100.0	0.0	STM0267	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_14	99.841	0.0	STM0268	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_15	100.0	1.42E-121	STM0269	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_16	98.905	0.0	STM0270	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_18	99.09	0.0	STM0272	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_19	98.889	6.15E-129	STM0273	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_20	99.801	0.0	STM0274	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_22	100.0	2.36E-121	STM0276	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_23	100.0	2.56E-120	tae4	VF1195	SCI T6SS secreted effectors	Effector delivery system	VFC0086		(tae4) type VI secretion system effector tae4, L,D-endopeptidase [SCI T6SS secreted effectors (VF1195) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000021.1_24	99.187	4.33E-90	STM0278	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_25	100.0	1.32E-120	STM0279	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_26	99.438	1.25E-131	tssJ	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_27	100.0	0.0	tssK	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_28	99.539	0.0	STM0282	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_29	83.984	1.09E-166	STM0283	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_31	99.612	0.0	STM0285	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_32	98.039	0.0	STM0286	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_35	100.0	1.84E-96	STM0287	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_36	100.0	5.13E-130	tlde1	VF1195	SCI T6SS secreted effectors	Effector delivery system	VFC0086		(tlde1) type VI secretion system effector tlde1, L,D-transpeptidase [SCI T6SS secreted effectors (VF1195) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000021.1_37	86.573	0.0	vgrG	VF0974	SCI (Salmonella centrisome island)/SPI-6 T6SS	Effector delivery system	VFC0086	"The T6SS is widely distributed in all Salmonella species and subspecies.; Salmonella T6SSs are located on five different Salmonella pathogenicity island and phylogenetically belong to i1,
LAZB01000021.1_52	100.0	1.79E-178	pagN	VF0968	PagN	Invasion	VFC0083	Unlike rck, pagN is encoded on bacterial chromosome.;PagN is well conserved and widely distributed among the different species and subspecies of Salmonella.;PagN protein displays similarity to the Hek and Tia invasins/adhesins of pathogenic E. coli	(pagN) outer membrane adhesin/invasin protein [PagN (VF0968) - Invasion (VFC0083)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000021.1_56	76.042	9.67E-111	gmhA/lpcA	VF0044	LOS	Immune modulation	VFC0258	Lic1A (phosphorylcholine (ChoP) kinase) 5'-CAAT-3' within the 5'-end of its coding sequence; lic2A, also referred to as lexA, variation in the number of 5'-CAAT-3' repeats has been shown to correlate directly with phase variation of the Gal-alpha(1-4)beta-Gal LPS structure; But lgtC (glycosyltransferase), another phase-variable gene, ultimately dictates whether this structure is synthesized. lic3A encode a sialyl transferase which directs the substitution of LPS with sialic acid.	(gmhA/lpcA) phosphoheptose isomerase [LOS (VF0044) - Immune modulation (VFC0258)] [Haemophilus influenzae Rd KW20]	Haemophilus influenzae
LAZB01000003.1_19	64.833	0.0	acrB	VF0568	AcrAB	Antimicrobial activity/Competitive advantage	VFC0325		(acrB) acriflavine resistance protein B [AcrAB (VF0568) - Antimicrobial activity/Competitive advantage (VFC0325)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000003.1_71	93.736	0.0	shdA	VF0398	ShdA	Adherence	VFC0001	The shdA gene is carried on a 25-kb genetic island at centisome 54 (CS54 island) of the Salmonella enterica serotype Typhimurium chromosome.	(shdA) AIDA autotransporter-like protein [ShdA (VF0398) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000003.1_72	68.367	0.0	shdA	VF0398	ShdA	Adherence	VFC0001	The shdA gene is carried on a 25-kb genetic island at centisome 54 (CS54 island) of the Salmonella enterica serotype Typhimurium chromosome.	(shdA) AIDA autotransporter-like protein [ShdA (VF0398) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000003.1_75	99.315	0.0	sinH	VF0400	SinH	Adherence	VFC0001	N-terminal 350 residues exhibits homology with invasin of Yersinia pseudotuberculosis (49.5% identity) and intimin of E. coli O111 (enteropathogenic E. coli) (48% identity). The amino termini of invasin and intimin serve as membrane-spanning anchors in the bacterial outer membrane.	(sinH) intimin-like protein [SinH (VF0400) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000003.1_146	65.445	1.05E-90	algU	VF0091	Alginate	Biofilm	VFC0271	Alginate production is frequently referred to as mucoidy because colonies producing alginate have a wet glistening (mucoid) appearance, which is very different from that of colonies not producing alginate; most of the alginate biosynthetic genes are clustered in the algD operon; Alginate production is highly regulated. Regulatory genes are located in two areas far removed from the biosynthetic genes, with one exception algC	(algU) alginate biosynthesis protein AlgZ/FimS [Alginate (VF0091) - Biofilm (VFC0271)] [Pseudomonas aeruginosa PAO1]	Pseudomonas aeruginosa
LAZB01000023.1_18	98.81	0.0	sseK1	VF0947	TTSS-2 secreted effectors	Effector delivery system	VFC0086		(sseK1) type III secretion system effector SseK1, Arginine N-Glycosyltransferase [TTSS-2 secreted effectors (VF0947) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000023.1_30	82.609	9.47E-70	tufA	VF0460	EF-Tu	Adherence	VFC0001		(tufA) elongation factor Tu [EF-Tu (VF0460) - Adherence (VFC0001)] [Francisella tularensis subsp. tularensis SCHU S4]	Francisella tularensis
LAZB01000026.1_27	96.34	0.0	slrP	VF0948	TTSS effectors secreted via both systems	Effector delivery system	VFC0086		(slrP) type III secretion system effector SlrP (Salmonella leucine-rich repeat protein),novel E3 ubiquitin ligase [TTSS effectors secreted via both systems (VF0948) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000004.1_113	88.908	0.0	ibeC	VF0237	Ibes	Invasion	VFC0083	IbeA is unique to E. coli K1. The ibeB and ibeC are found to have K12 homologues p77211 and yijP respectively.	(ibeC) phosphoethanolamine transferase CptA [Ibes (VF0237) - Invasion (VFC0083)] [Escherichia coli O45:K1:H7 str. S88]	Escherichia coli (NMEC)
LAZB01000029.1_4	64.721	5.2E-179	lpxB	VF0044	LOS	Immune modulation	VFC0258	Lic1A (phosphorylcholine (ChoP) kinase) 5'-CAAT-3' within the 5'-end of its coding sequence; lic2A, also referred to as lexA, variation in the number of 5'-CAAT-3' repeats has been shown to correlate directly with phase variation of the Gal-alpha(1-4)beta-Gal LPS structure; But lgtC (glycosyltransferase), another phase-variable gene, ultimately dictates whether this structure is synthesized. lic3A encode a sialyl transferase which directs the substitution of LPS with sialic acid.	(lpxB) lipid-A-disaccharide synthase [LOS (VF0044) - Immune modulation (VFC0258)] [Haemophilus influenzae Rd KW20]	Haemophilus influenzae
LAZB01000029.1_5	67.939	4.76E-131	lpxA	VF0044	LOS	Immune modulation	VFC0258	Lic1A (phosphorylcholine (ChoP) kinase) 5'-CAAT-3' within the 5'-end of its coding sequence; lic2A, also referred to as lexA, variation in the number of 5'-CAAT-3' repeats has been shown to correlate directly with phase variation of the Gal-alpha(1-4)beta-Gal LPS structure; But lgtC (glycosyltransferase), another phase-variable gene, ultimately dictates whether this structure is synthesized. lic3A encode a sialyl transferase which directs the substitution of LPS with sialic acid.	(lpxA) UDP-N-acetylglucosamine acyltransferase [LOS (VF0044) - Immune modulation (VFC0258)] [Haemophilus influenzae Rd KW20]	Haemophilus influenzae
LAZB01000029.1_7	64.497	3.48E-159	lpxD	VF0044	LOS	Immune modulation	VFC0258	Lic1A (phosphorylcholine (ChoP) kinase) 5'-CAAT-3' within the 5'-end of its coding sequence; lic2A, also referred to as lexA, variation in the number of 5'-CAAT-3' repeats has been shown to correlate directly with phase variation of the Gal-alpha(1-4)beta-Gal LPS structure; But lgtC (glycosyltransferase), another phase-variable gene, ultimately dictates whether this structure is synthesized. lic3A encode a sialyl transferase which directs the substitution of LPS with sialic acid.	(lpxD) UDP-3-O-(3-hydroxymyristoyl) glucosamine N-acyltransferase [LOS (VF0044) - Immune modulation (VFC0258)] [Haemophilus influenzae Rd KW20]	Haemophilus influenzae
LAZB01000029.1_107	77.303	0.0	lpxC	VF0044	LOS	Immune modulation	VFC0258	Lic1A (phosphorylcholine (ChoP) kinase) 5'-CAAT-3' within the 5'-end of its coding sequence; lic2A, also referred to as lexA, variation in the number of 5'-CAAT-3' repeats has been shown to correlate directly with phase variation of the Gal-alpha(1-4)beta-Gal LPS structure; But lgtC (glycosyltransferase), another phase-variable gene, ultimately dictates whether this structure is synthesized. lic3A encode a sialyl transferase which directs the substitution of LPS with sialic acid.	(lpxC) UDP-3-O-(R-3-hydroxymyristoyl)-N-acetylglucosamine deacetylase [LOS (VF0044) - Immune modulation (VFC0258)] [Haemophilus influenzae Rd KW20]	Haemophilus influenzae
LAZB01000029.1_298	72.352	0.0	cheD	VF0394	Flagella	Motility	VFC0204		(cheD) methyl-accepting chemotaxis protein CheD [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000029.1_404	99.553	0.0	srfJ	VF0947	TTSS-2 secreted effectors	Effector delivery system	VFC0086		(srfJ) type III secretion system Effector SrfJ, glucosylceramidase activity [TTSS-2 secreted effectors (VF0947) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000029.1_497	75.758	0.0	htpB	VF0159	Hsp60	Adherence	VFC0001		(htpB) Hsp60, 60K heat shock protein HtpB [Hsp60 (VF0159) - Adherence (VFC0001)] [Legionella pneumophila subsp. pneumophila str. Philadelphia 1]	Legionella pneumophila
LAZB01000029.1_558	100.0	4.18E-165	pmrA	VF1355	PmrAB	Regulation	VFC0301		(pmrA) response regulator PmrA [PmrAB (VF1355) - Regulation (VFC0301)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000029.1_559	100.0	0.0	pmrB	VF1355	PmrAB	Regulation	VFC0301		(pmrB) sensory kinase PmrB [PmrAB (VF1355) - Regulation (VFC0301)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000029.1_590	97.716	0.0	siiE	VF0970	SiiE	Adherence	VFC0001	SiiE is located within Salmonella Pathogenicity Island SPI-4, a 27-kb region that carries six genes designated siiABCDEF. SiiC, SiiD, and SiiF form a type I secretion apparatus for the secretion of SiiE.;With 595 kDa, SiiE is the largest protein of the Salmonella proteome.;SiiE, like many other non-fimbrial adhesins binds to glycostructures at the cell surface.	(siiE) non-fimbrial adhesin SiiE [SiiE (VF0970) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000029.1_615	69.748	2.15E-124	sopE2	VF0949	TTSS-1 secreted effectors	Effector delivery system	VFC0086		(sopE2) type III secretion system effector SopE2, guanine nucleotide exchange factor [TTSS-1 secreted effectors (VF0949) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000029.1_704	84.437	0.0	gtrB	VF0124	LPS	Immune modulation	VFC0258	Composed of the O-antigen, core polysaccharides and lipid A; the genes involved in the biosynthesis of the basic O-antigen are located in the rfb/rfc loci; O-antigen modification is associated with temperate bacteriophages. Four different serotype-converting phages have been found: SfII, Sf6, SfV and SfX, which are involved in conversion of a serotype Y stain to serotypes 2a, 3b, 5a and X, respectively	(gtrB) bactoprenol glucosyl transferase [LPS (VF0124) - Immune modulation (VFC0258)] [Shigella flexneri 2a str. 301]	Shigella flexneri
LAZB01000029.1_723	61.827	0.0	icl	VF0253	Isocitrate lyase	Others	VFC0346		(icl) Isocitrate lyase Icl (isocitrase) (isocitratase) [Isocitrate lyase (VF0253) - Others (VFC0346)] [Mycobacterium tuberculosis H37Rv]	Mycobacterium tuberculosis
LAZB01000005.1_4	75.0	3.37E-161	galU	VF0044	LOS	Immune modulation	VFC0258	Lic1A (phosphorylcholine (ChoP) kinase) 5'-CAAT-3' within the 5'-end of its coding sequence; lic2A, also referred to as lexA, variation in the number of 5'-CAAT-3' repeats has been shown to correlate directly with phase variation of the Gal-alpha(1-4)beta-Gal LPS structure; But lgtC (glycosyltransferase), another phase-variable gene, ultimately dictates whether this structure is synthesized. lic3A encode a sialyl transferase which directs the substitution of LPS with sialic acid.	(galU) glucosephosphate uridylyltransferase [LOS (VF0044) - Immune modulation (VFC0258)] [Haemophilus influenzae Rd KW20]	Haemophilus influenzae
LAZB01000005.1_22	81.915	1.9E-178	kdsA	VF0044	LOS	Immune modulation	VFC0258	Lic1A (phosphorylcholine (ChoP) kinase) 5'-CAAT-3' within the 5'-end of its coding sequence; lic2A, also referred to as lexA, variation in the number of 5'-CAAT-3' repeats has been shown to correlate directly with phase variation of the Gal-alpha(1-4)beta-Gal LPS structure; But lgtC (glycosyltransferase), another phase-variable gene, ultimately dictates whether this structure is synthesized. lic3A encode a sialyl transferase which directs the substitution of LPS with sialic acid.	(kdsA) 2-dehydro-3-deoxyphosphooctonate aldolase [LOS (VF0044) - Immune modulation (VFC0258)] [Haemophilus influenzae Rd KW20]	Haemophilus influenzae
LAZB01000005.1_105	96.667	2.39E-177	sopE2	VF0949	TTSS-1 secreted effectors	Effector delivery system	VFC0086		(sopE2) type III secretion system effector SopE2, guanine nucleotide exchange factor [TTSS-1 secreted effectors (VF0949) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_110	76.244	0.0	sspH2	VF0947	TTSS-2 secreted effectors	Effector delivery system	VFC0086		(sspH2) type III secretion system effector SspH2 (Salmonella secreted protein H2), novel E3 ubiquitin ligase [TTSS-2 secreted effectors (VF0947) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_139	60.494	6.26E-107	CBU_1566	VF0696	T4SS secreted effectors	Effector delivery system	VFC0086		(CBU_1566) Coxiella Dot/Icm type IVB secretion system translocated effector [T4SS secreted effectors (VF0696) - Effector delivery system (VFC0086)] [Coxiella burnetii RSA 493]	Coxiella burnetii
LAZB01000005.1_153	85.507	0.0	flhA	VF0394	Flagella	Motility	VFC0204		(flhA) flagellar biosynthesis protein FlhA [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_154	66.053	0.0	flhB	VF0394	Flagella	Motility	VFC0204		(flhB) flagellar biosynthetic protein FlhB [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_155	78.641	5.68E-111	cheZ	VF0394	Flagella	Motility	VFC0204		(cheZ) chemotaxis regulator CheZ [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_156	90.698	5.38E-84	cheY	VF0394	Flagella	Motility	VFC0204		(cheY) chemotaxis regulatory protein CheY [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_157	85.387	0.0	cheB	VF0394	Flagella	Motility	VFC0204		(cheB) chemotaxis-specific methylesterase CheB [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_158	73.944	3.46E-152	cheR	VF0394	Flagella	Motility	VFC0204		(cheR) chemotaxis methyltransferase CheR [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_160	85.0	2.26E-97	cheW	VF0394	Flagella	Motility	VFC0204		(cheW) purine-binding chemotaxis protein CheW [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_161	75.811	0.0	cheA	VF0394	Flagella	Motility	VFC0204		(cheA) chemotaxis protein CheA [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_162	68.571	3.59E-154	motB	VF0394	Flagella	Motility	VFC0204		(motB) flagellar motor protein MotB [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_163	83.051	0.0	motA	VF0394	Flagella	Motility	VFC0204		(motA) flagellar motor protein MotA [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_164	81.865	1.31E-116	flhC	VF0394	Flagella	Motility	VFC0204		(flhC) flagellar biosynthesis transcription activator FlhC [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_165	75.862	5.28E-53	flhD	VF0394	Flagella	Motility	VFC0204		(flhD) flagellar transcriptional activator FlhD [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_190	83.193	9.01E-144	fliA	VF0394	Flagella	Motility	VFC0204		(fliA) flagellar biosynthesis sigma factor [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_194	71.094	1.59E-62	fliS	VF0394	Flagella	Motility	VFC0204		(fliS) flagellar protein FliS [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_202	63.321	0.0	fliF	VF0394	Flagella	Motility	VFC0204		(fliF) flagellar M-ring protein FliF [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_203	83.283	0.0	fliG	VF0394	Flagella	Motility	VFC0204		(fliG) flagellar motor switch protein G [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_205	84.141	0.0	fliI	VF0394	Flagella	Motility	VFC0204		(fliI) flagellum-specific ATP synthase FliI [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_209	84.985	0.0	fliM	VF0394	Flagella	Motility	VFC0204		(fliM) flagellar motor switch protein FliM [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_210	76.812	7.21E-71	fliN	VF0394	Flagella	Motility	VFC0204		(fliN) flagellar motor switch protein FliN [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_212	85.652	1.94E-141	fliP	VF0394	Flagella	Motility	VFC0204		(fliP) flagellar biosynthetic protein FliP [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_213	74.157	2.47E-36	fliQ	VF0394	Flagella	Motility	VFC0204		(fliQ) flagellar biosynthetic protein FliQ [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_214	65.891	2.28E-103	fliR	VF0394	Flagella	Motility	VFC0204		(fliR) flagellar biosynthetic protein FliR [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_215	65.217	1.71E-99	rcsA	VF0571	RcsAB	Regulation	VFC0301		(rcsA) transcriptional activator for ctr capsule biosynthesis [RcsAB (VF0571) - Regulation (VFC0301)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000005.1_313	97.326	0.0	sopB/sigD	VF0949	TTSS-1 secreted effectors	Effector delivery system	VFC0086		(sopB/sigD) type III secretion system effector SopB, phosphoinositide phosphatase [TTSS-1 secreted effectors (VF0949) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_315	96.907	0.0	pipB	VF0947	TTSS-2 secreted effectors	Effector delivery system	VFC0086		(pipB) type III secretion system effector PipB [TTSS-2 secreted effectors (VF0947) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_332	92.857	0.0	ompA	VF0236	OmpA	Invasion	VFC0083	Major outer membrane protein in E. coli, homologous to Neisseria Opa proteins which have been shown to be involved in invasion of eukaryotic cells	(ompA) outer membrane protein A [OmpA (VF0236) - Invasion (VFC0083)] [Escherichia coli O18:K1:H7 str. RS218]	Escherichia coli (NMEC)
LAZB01000005.1_361	69.478	2.28E-125	nueA	VF0473	Polar flagella	Motility	VFC0204	Types of bacterial movement: swimming, swarming, gliding, twitching and sliding. Only swimming and swarming are correlated with the presence of flagella. Swimming is an individual endeavour, while swarming is the movement of a group of bacteria; constitutively expressed for motility in liquid environments	(nueA) NeuA protein [Polar flagella (VF0473) - Motility (VFC0204)] [Aeromonas hydrophila ML09-119]	Aeromonas hydrophila
LAZB01000005.1_365	66.263	0.0	msbA	VF0044	LOS	Immune modulation	VFC0258	Lic1A (phosphorylcholine (ChoP) kinase) 5'-CAAT-3' within the 5'-end of its coding sequence; lic2A, also referred to as lexA, variation in the number of 5'-CAAT-3' repeats has been shown to correlate directly with phase variation of the Gal-alpha(1-4)beta-Gal LPS structure; But lgtC (glycosyltransferase), another phase-variable gene, ultimately dictates whether this structure is synthesized. lic3A encode a sialyl transferase which directs the substitution of LPS with sialic acid.	(msbA) lipid transporter ATP-binding/permease [LOS (VF0044) - Immune modulation (VFC0258)] [Haemophilus influenzae Rd KW20]	Haemophilus influenzae
LAZB01000005.1_377	91.223	0.0	sopD2	VF0947	TTSS-2 secreted effectors	Effector delivery system	VFC0086		(sopD2) type III secretion system effector SopD2 [TTSS-2 secreted effectors (VF0947) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_532	92.341	0.0	steC	VF0947	TTSS-2 secreted effectors	Effector delivery system	VFC0086		(steC) type III secretion system effector SteC (Salmonella translocated effector C), kinase [TTSS-2 secreted effectors (VF0947) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_607	94.608	0.0	sseJ	VF0947	TTSS-2 secreted effectors	Effector delivery system	VFC0086		(sseJ) type III secretion system effector SseJ, glycerophospholipid:cholesterol acyltransferase [TTSS-2 secreted effectors (VF0947) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_636	93.987	0.0	sifB	VF0947	TTSS-2 secreted effectors	Effector delivery system	VFC0086		(sifB) type III secretion system effector SifB (Salmonella induced filament protein B) [TTSS-2 secreted effectors (VF0947) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_654	88.095	5.4E-138	steA	VF0948	TTSS effectors secreted via both systems	Effector delivery system	VFC0086		(steA) type III secretion system effector SteA (Salmonella translocated effector A) [TTSS effectors secreted via both systems (VF0948) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_822	68.063	3.66E-100	sodB	VF0169	SodB	Stress survival	VFC0282		(sodB) superoxide dismutase [SodB (VF0169) - Stress survival (VFC0282)] [Legionella pneumophila subsp. pneumophila str. Philadelphia 1]	Legionella pneumophila
LAZB01000005.1_830	99.716	0.0	ssaU	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaU) type III secretion system export apparatus switch protein SsaU [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_831	97.297	0.0	ssaT	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaT) type III secretion system minor export apparatus protein SsaT [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_832	100.0	7.18E-59	ssaS	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaS) type III secretion system minor export apparatus protein SsaS [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_833	100.0	1.64E-153	ssaR	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaR) type III secretion system minor export apparatus protein SsaR [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_834	97.826	0.0	ssaQ	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaQ) type III secretion system C ring protein SsaQ [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_835	97.581	9.38E-91	ssaP	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaP) type III secretion system needle length regulator SsaP [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_836	100.0	7.09E-88	ssaO	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaO) type III secretion system stalk protein SsaO [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_837	99.538	0.0	ssaN	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaN) type III secretion system ATPase SsaN [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_838	99.413	0.0	ssaV	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaV) type III secretion system major export apparatus protein ssaV [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_839	96.721	1.57E-87	ssaM	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaM) type III secretion system protein SsaM [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_840	99.091	0.0	ssaL	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaL) type III secretion system gatekeeper SsaL [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_841	99.107	4.97E-167	ssaK	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaK) type III secretion system stator SsaK [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_842	97.59	4.5E-55	ssaX	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaX) type III secretion system base-pod connector [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_843	98.605	4.41E-159	ssaJ	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaJ) type III secretion system inner MS ring protein SsaJ [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_844	98.765	5.28E-55	ssaI	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaI) type III secretion system inner rod protein SsaI [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_846	100.0	1.02E-47	ssaG	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaG) type III secretion system needle filament protein SsaG [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_847	99.127	1.8E-171	sseG	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(sseG) type III secretion system effector SseG [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_848	96.538	0.0	sseF	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(sseF) type III secretion system effector SseF [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_849	99.296	6.3E-106	sscB	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(sscB) chaperone for sseF [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_850	100.0	4.77E-100	sseE	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(sseE) type III secretion system effector SseE [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_851	94.359	2.52E-132	sseD	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(sseD) type III secretion system hydrophilic translocator, pore protein SseD [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_852	91.322	0.0	sseC	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(sseC) type III secretion system hydrophilic translocator, pore protein SseC [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_853	98.726	3.84E-116	sscA	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(sscA) chaperone for sseC [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_854	96.939	2.04E-140	sseB	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(sseB) type III secretion system effector SseB [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_855	98.131	6.69E-75	sseA	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(sseA) chaperone for sseB and sseD [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_856	97.5	5.34E-52	ssaE	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaE) chaperone for sseB [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_857	99.256	0.0	ssaD	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaD) type III secretion system outer MS ring protein SsaD [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_858	99.195	0.0	ssaC	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssaC) type III secretion system secretin SsaC [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_859	99.213	1.66E-92	spiC/ssaB	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(spiC/ssaB) Salmonella pathogenicity island 2 protein C (SpiC); Type III secretion system apparatus protein B (SsaB) [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_860	98.804	0.0	ssrA	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssrA) hybrid sensor histidine kinase/response regulator [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_861	99.528	3.35E-158	ssrB	VF0321	TTSS (SPI-2 encode)	Effector delivery system	VFC0086	SPI-2 T3SS effector repertoire varies greatly among different Salmonella serovars.; All serovars seem to have a set of 'core' effectors (SseF, SseG, PipB, SteA, SifA, SteD and PipB2), suggesting that they are critical for virulence in different hosts.; Another group of effectors (SseL, SifB, SopD2, SseJ, SteB, SteC, SlrP, and SseK2) always seem to be present in intestinal serovars but are frequently non-functional in extraintestinal or highly host-adapted serovars, suggesting these effectors contribute to virulence in the intestine, but not always in deeper tissues.;A further group of 'accessory' effectors (SspH2, SseK1, SrfJ, GtgA, GtgE, SseI, GogB, SteE, SseK3, SspH1, SpvB, SpvC, and SpvD) encoded on mobile genetic elements (MGEs) or DNA close to the remnants of MGEs are found sporadically across different serovars.;The only known effector genes in SPI-2, sseF and sseG, are likely to have conferred an early selective advantage to intracellular bacteria.;several sets of effectors that share high levels of sequence similarity. Examples of paralog effectors include Pathogenicity island-encoded protein B (PipB) and PipB2, which share 33% identity and 67% similarity, SifA and SifB that share 26% identity and 46% similarity, SopE and SopE2, which share 69% similarity, SopD and SopD2 that share 43% identity and 63% similarity. These effector protein paralogs often share structural similarity and/or biochemical activities but demonstrate functional divergence in intracellular localization and/or host protein targets or interaction partners.	(ssrB) DNA-binding response regulator [TTSS (SPI-2 encode) (VF0321) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_1017	100.0	1.34E-166	phoP	VF0111	PhoPQ	Regulation	VFC0301		(phoP) response regulator in two-component regulatory system with PhoQ [PhoPQ (VF0111) - Regulation (VFC0301)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_1018	100.0	0.0	phoQ	VF0111	PhoPQ	Regulation	VFC0301		(phoQ) sensor protein PhoQ [PhoPQ (VF0111) - Regulation (VFC0301)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_1024	89.881	0.0	sifA	VF0947	TTSS-2 secreted effectors	Effector delivery system	VFC0086		(sifA) type III secretion system effector SifA (Salmonella induced filament protein A) [TTSS-2 secreted effectors (VF0947) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_1052	61.538	1.93E-27	acpXL	VF0367	LPS	Immune modulation	VFC0258	Brucella possesses a non-classical LPS as compared with the so-called classical LPS from enterobacteria such as Escherichia coli. B. abortus lipid A possesses a diaminoglucose backbone (rather than glucosamine), and acyl groups are longer (C28 rather than C12 and C16) and are only linked to the core by amide bounds (rather than ester and amide bonds).; In contrast to enterobacterial LPSs, Brucella LPS is several-hundred-times less active and toxic than E. coli LPS.; this is an evolutionary adaptation to an intracellular lifestyle, low endotoxic activity is shared by other intracellular pathogens such as Bartonella and Legionella.	(acpXL) acyl carrier protein [LPS (VF0367) - Immune modulation (VFC0258)] [Brucella melitensis bv. 1 str. 16M]	Brucella melitensis
LAZB01000005.1_1053	77.459	1.72E-139	flmH	VF0473	Polar flagella	Motility	VFC0204	Types of bacterial movement: swimming, swarming, gliding, twitching and sliding. Only swimming and swarming are correlated with the presence of flagella. Swimming is an individual endeavour, while swarming is the movement of a group of bacteria; constitutively expressed for motility in liquid environments	(flmH) short chain dehydrogenase/reductase family oxidoreductase [Polar flagella (VF0473) - Motility (VFC0204)] [Aeromonas hydrophila ML09-119]	Aeromonas hydrophila
LAZB01000005.1_1066	61.146	2.38E-137	flgJ	VF0394	Flagella	Motility	VFC0204		(flgJ) <beta>-N-acetylglucosaminidase [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_1067	79.05	0.0	flgI	VF0394	Flagella	Motility	VFC0204		(flgI) flagellar P-ring protein precursor FlgI [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_1068	82.16	4.37E-122	flgH	VF0394	Flagella	Motility	VFC0204		(flgH) flagellar L-ring protein precursor FlgH [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_1069	87.308	5.49E-170	flgG	VF0394	Flagella	Motility	VFC0204		(flgG) flagellar basal-body rod protein FlgG [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_1070	69.721	8.16E-126	flgF	VF0394	Flagella	Motility	VFC0204		(flgF) flagellar basal-body rod protein FlgF [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_1071	63.183	2.55E-180	flgE	VF0394	Flagella	Motility	VFC0204		(flgE) flagellar hook protein FlgE [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_1072	71.287	9.94E-99	flgD	VF0394	Flagella	Motility	VFC0204		(flgD) flagellar basal-body rod modification protein FlgD [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_1073	81.343	1.88E-80	flgC	VF0394	Flagella	Motility	VFC0204		(flgC) flagellar basal-body rod protein FlgC [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_1074	76.642	3.3E-76	flgB	VF0394	Flagella	Motility	VFC0204		(flgB) flagellar basal-body rod protein FlgB [Flagella (VF0394) - Motility (VFC0204)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_1104	100.0	5.6E-75	csgC	VF0103	Agf	Adherence	VFC0001	Homology to csg of E.coli; nucleator-dependent assembly pathway	(csgC) curli assembly protein CsgC [Agf (VF0103) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_1105	100.0	3.01E-106	csgA	VF0103	Agf	Adherence	VFC0001	Homology to csg of E.coli; nucleator-dependent assembly pathway	(csgA) curlin major subunit CsgA [Agf (VF0103) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_1106	100.0	1.03E-108	csgB	VF0103	Agf	Adherence	VFC0001	Homology to csg of E.coli; nucleator-dependent assembly pathway	(csgB) minor curlin subunit precursor, curli nucleator protein CsgB [Agf (VF0103) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_1107	100.0	8.63E-164	csgD	VF0103	Agf	Adherence	VFC0001	Homology to csg of E.coli; nucleator-dependent assembly pathway	(csgD) DNA-binding transcriptional regulator CsgD [Agf (VF0103) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_1108	100.0	1.59E-96	csgE	VF0103	Agf	Adherence	VFC0001	Homology to csg of E.coli; nucleator-dependent assembly pathway	(csgE) curli production assembly/transport protein CsgE [Agf (VF0103) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_1109	100.0	2.24E-100	csgF	VF0103	Agf	Adherence	VFC0001	Homology to csg of E.coli; nucleator-dependent assembly pathway	(csgF) curli production assembly/transport protein CsgF [Agf (VF0103) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_1110	100.0	0.0	csgG	VF0103	Agf	Adherence	VFC0001	Homology to csg of E.coli; nucleator-dependent assembly pathway	(csgG) curli production assembly/transport protein CsgG [Agf (VF0103) - Adherence (VFC0001)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_1226	97.57	0.0	sopA	VF0949	TTSS-1 secreted effectors	Effector delivery system	VFC0086		(sopA) type III secretion system effector SopA, HECT-like E3 ubiquitin ligase [TTSS-1 secreted effectors (VF0949) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_1240	81.959	0.0	ugd	VF0560	Capsule	Immune modulation	VFC0258	The Klebsiella polysaccharide capsule is produced through a Wzy-dependent process, for which the synthesis and export machinery are encoded in a single 10-30 kb region of the genome known as the K locus.; 78 distinct capsule phenotypes have been recognized by serological typing, but many isolates are serologically non-typable.; capsular serotypes vary substantially in the degree of serum resistance; K1, K2 and K5 are highly serum resistant and are associated with hypervirulent strains that differ from classical K. pneumoniae in that they commonly cause community-acquired disease.	(ugd) UDP-glucose 6-dehydrogenase [Capsule (VF0560) - Immune modulation (VFC0258)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000005.1_1241	95.513	0.0	gndA	VF0560	Capsule	Immune modulation	VFC0258	The Klebsiella polysaccharide capsule is produced through a Wzy-dependent process, for which the synthesis and export machinery are encoded in a single 10-30 kb region of the genome known as the K locus.; 78 distinct capsule phenotypes have been recognized by serological typing, but many isolates are serologically non-typable.; capsular serotypes vary substantially in the degree of serum resistance; K1, K2 and K5 are highly serum resistant and are associated with hypervirulent strains that differ from classical K. pneumoniae in that they commonly cause community-acquired disease.	(gndA) NADP-dependent phosphogluconate dehydrogenase [Capsule (VF0560) - Immune modulation (VFC0258)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000005.1_1251	69.944	0.0	rfbG	VF0392	O-antigen	Immune modulation	VFC0258	Clinical Y. enterocolitica isolates from humans predominantly belong to serotypes O:3, O:9, O:8 and O:5,27; Y. enterocolitica O antigen expression is temperature regulated.	(rfbG) CDP-glucose 4,6-dehydratase [O-antigen (VF0392) - Immune modulation (VFC0258)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_1252	79.377	3.74E-162	rfbF	VF0392	O-antigen	Immune modulation	VFC0258	Clinical Y. enterocolitica isolates from humans predominantly belong to serotypes O:3, O:9, O:8 and O:5,27; Y. enterocolitica O antigen expression is temperature regulated.	(rfbF) glucose-1-phosphate cytidylyltransferase [O-antigen (VF0392) - Immune modulation (VFC0258)] [Yersinia enterocolitica subsp. enterocolitica 8081]	Yersinia enterocolitica
LAZB01000005.1_1255	63.103	1.31E-140	wbtL	VF0542	LPS	Immune modulation	VFC0258	The structure of Francisella spp. lipid A is unique in that it is modified by various carbohydrates that greatly reduce TLR4 activation and allow for immune evasion	(wbtL) glucose-1-phosphate thymidylyltransferase [LPS (VF0542) - Immune modulation (VFC0258)] [Francisella tularensis subsp. tularensis SCHU S4]	Francisella tularensis
LAZB01000005.1_1257	62.573	1.69E-159	rffG	VF0044	LOS	Immune modulation	VFC0258	Lic1A (phosphorylcholine (ChoP) kinase) 5'-CAAT-3' within the 5'-end of its coding sequence; lic2A, also referred to as lexA, variation in the number of 5'-CAAT-3' repeats has been shown to correlate directly with phase variation of the Gal-alpha(1-4)beta-Gal LPS structure; But lgtC (glycosyltransferase), another phase-variable gene, ultimately dictates whether this structure is synthesized. lic3A encode a sialyl transferase which directs the substitution of LPS with sialic acid.	(rffG) dTDP-glucose 46-dehydratase [LOS (VF0044) - Immune modulation (VFC0258)] [Haemophilus influenzae Rd KW20]	Haemophilus influenzae
LAZB01000005.1_1258	92.542	0.0	galF	VF0560	Capsule	Immune modulation	VFC0258	The Klebsiella polysaccharide capsule is produced through a Wzy-dependent process, for which the synthesis and export machinery are encoded in a single 10-30 kb region of the genome known as the K locus.; 78 distinct capsule phenotypes have been recognized by serological typing, but many isolates are serologically non-typable.; capsular serotypes vary substantially in the degree of serum resistance; K1, K2 and K5 are highly serum resistant and are associated with hypervirulent strains that differ from classical K. pneumoniae in that they commonly cause community-acquired disease.	(galF) GalU regulator GalF [Capsule (VF0560) - Immune modulation (VFC0258)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000005.1_1263	64.026	0.0	wcaJ	VF0560	Capsule	Immune modulation	VFC0258	The Klebsiella polysaccharide capsule is produced through a Wzy-dependent process, for which the synthesis and export machinery are encoded in a single 10-30 kb region of the genome known as the K locus.; 78 distinct capsule phenotypes have been recognized by serological typing, but many isolates are serologically non-typable.; capsular serotypes vary substantially in the degree of serum resistance; K1, K2 and K5 are highly serum resistant and are associated with hypervirulent strains that differ from classical K. pneumoniae in that they commonly cause community-acquired disease.	(wcaJ) undecaprenyl-phosphate glucose phosphotransferase [Capsule (VF0560) - Immune modulation (VFC0258)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000005.1_1264	76.754	0.0	rfbK1	VF0560	Capsule	Immune modulation	VFC0258	The Klebsiella polysaccharide capsule is produced through a Wzy-dependent process, for which the synthesis and export machinery are encoded in a single 10-30 kb region of the genome known as the K locus.; 78 distinct capsule phenotypes have been recognized by serological typing, but many isolates are serologically non-typable.; capsular serotypes vary substantially in the degree of serum resistance; K1, K2 and K5 are highly serum resistant and are associated with hypervirulent strains that differ from classical K. pneumoniae in that they commonly cause community-acquired disease.	(rfbK1) O9 family phosphomannomutase RfbK1 [Capsule (VF0560) - Immune modulation (VFC0258)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000005.1_1265	62.076	0.0	KP1_RS17280	VF0560	Capsule	Immune modulation	VFC0258	The Klebsiella polysaccharide capsule is produced through a Wzy-dependent process, for which the synthesis and export machinery are encoded in a single 10-30 kb region of the genome known as the K locus.; 78 distinct capsule phenotypes have been recognized by serological typing, but many isolates are serologically non-typable.; capsular serotypes vary substantially in the degree of serum resistance; K1, K2 and K5 are highly serum resistant and are associated with hypervirulent strains that differ from classical K. pneumoniae in that they commonly cause community-acquired disease.	(KP1_RS17280) mannose-1-phosphate guanylyltransferase/mannose-6-phosphate isomerase [Capsule (VF0560) - Immune modulation (VFC0258)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000005.1_1266	60.688	0.0	KP1_RS17295	VF0560	Capsule	Immune modulation	VFC0258	The Klebsiella polysaccharide capsule is produced through a Wzy-dependent process, for which the synthesis and export machinery are encoded in a single 10-30 kb region of the genome known as the K locus.; 78 distinct capsule phenotypes have been recognized by serological typing, but many isolates are serologically non-typable.; capsular serotypes vary substantially in the degree of serum resistance; K1, K2 and K5 are highly serum resistant and are associated with hypervirulent strains that differ from classical K. pneumoniae in that they commonly cause community-acquired disease.	(KP1_RS17295) glycosyltransferase WbuB [Capsule (VF0560) - Immune modulation (VFC0258)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000005.1_1268	76.489	0.0	KP1_RS17305	VF0560	Capsule	Immune modulation	VFC0258	The Klebsiella polysaccharide capsule is produced through a Wzy-dependent process, for which the synthesis and export machinery are encoded in a single 10-30 kb region of the genome known as the K locus.; 78 distinct capsule phenotypes have been recognized by serological typing, but many isolates are serologically non-typable.; capsular serotypes vary substantially in the degree of serum resistance; K1, K2 and K5 are highly serum resistant and are associated with hypervirulent strains that differ from classical K. pneumoniae in that they commonly cause community-acquired disease.	(KP1_RS17305) GDP-L-fucose synthase [Capsule (VF0560) - Immune modulation (VFC0258)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000005.1_1269	88.649	0.0	gmd	VF0560	Capsule	Immune modulation	VFC0258	The Klebsiella polysaccharide capsule is produced through a Wzy-dependent process, for which the synthesis and export machinery are encoded in a single 10-30 kb region of the genome known as the K locus.; 78 distinct capsule phenotypes have been recognized by serological typing, but many isolates are serologically non-typable.; capsular serotypes vary substantially in the degree of serum resistance; K1, K2 and K5 are highly serum resistant and are associated with hypervirulent strains that differ from classical K. pneumoniae in that they commonly cause community-acquired disease.	(gmd) GDP-mannose 4,6-dehydratase [Capsule (VF0560) - Immune modulation (VFC0258)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000005.1_1278	64.644	0.0	KP1_RS17340	VF0560	Capsule	Immune modulation	VFC0258	The Klebsiella polysaccharide capsule is produced through a Wzy-dependent process, for which the synthesis and export machinery are encoded in a single 10-30 kb region of the genome known as the K locus.; 78 distinct capsule phenotypes have been recognized by serological typing, but many isolates are serologically non-typable.; capsular serotypes vary substantially in the degree of serum resistance; K1, K2 and K5 are highly serum resistant and are associated with hypervirulent strains that differ from classical K. pneumoniae in that they commonly cause community-acquired disease.	(KP1_RS17340) polysaccharide export protein [Capsule (VF0560) - Immune modulation (VFC0258)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000005.1_1303	64.815	4.73E-16	rhs/PAAR	VF0579	T6SS	Effector delivery system	VFC0086		(rhs/PAAR) Type VI secretion system protein, PAAR family [T6SS (VF0579) - Effector delivery system (VFC0086)] [Shigella sonnei Ss046]	Shigella sonnei
LAZB01000005.1_1311	98.209	0.0	sseK2	VF0947	TTSS-2 secreted effectors	Effector delivery system	VFC0086		(sseK2) type III secretion system effector SseK2 [TTSS-2 secreted effectors (VF0947) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000005.1_1313	89.189	3.76E-61	steD	VF0947	TTSS-2 secreted effectors	Effector delivery system	VFC0086		(steD) type III secretion system effector SteD [TTSS-2 secreted effectors (VF0947) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000006.1_1	83.529	1.63E-48	tufA	VF0460	EF-Tu	Adherence	VFC0001		(tufA) elongation factor Tu [EF-Tu (VF0460) - Adherence (VFC0001)] [Francisella tularensis subsp. tularensis SCHU S4]	Francisella tularensis
LAZB01000006.1_22	67.327	4.54E-100	vfr	VF0082	Type IV pili	Adherence	VFC0001	PilA, B, C, D, E, F, M, N, O, P, Q, T, U, V, W, X, Y1, Y2, Z, and fimT, U, V are involved in the biogenesis and mechanical function of pili, pilG, H, I, K, chpA, B, C, D, E, pilS, R, fimS, rpoN, algR, algU, and vfr are involved in transcriptional regulation and chemosensory pathways that control the expression or activity of the twitching motility of the pili	(vfr) cAMP-regulatory protein [Type IV pili (VF0082) - Adherence (VFC0001)] [Pseudomonas aeruginosa PAO1]	Pseudomonas aeruginosa
LAZB01000006.1_38	63.964	1.04E-101	rpe	VF0543	Capsule	Immune modulation	VFC0258	Group 4 capsule; high molecular weight (HMW) O-antigen capsule	(rpe) ribulose-phosphate 3-epimerase [Capsule (VF0543) - Immune modulation (VFC0258)] [Francisella tularensis subsp. tularensis SCHU S4]	Francisella tularensis
LAZB01000007.1_101	68.533	0.0	acrA	VF0568	AcrAB	Antimicrobial activity/Competitive advantage	VFC0325		(acrA) acriflavine resistance protein A [AcrAB (VF0568) - Antimicrobial activity/Competitive advantage (VFC0325)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000007.1_102	80.845	0.0	acrB	VF0568	AcrAB	Antimicrobial activity/Competitive advantage	VFC0325		(acrB) acriflavine resistance protein B [AcrAB (VF0568) - Antimicrobial activity/Competitive advantage (VFC0325)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000008.1_17	97.685	5.01E-154	rcsB	VF0571	RcsAB	Regulation	VFC0301		(rcsB) transcriptional regulator RcsB [RcsAB (VF0571) - Regulation (VFC0301)] [Klebsiella pneumoniae subsp. pneumoniae NTUH-K2044]	Klebsiella pneumoniae
LAZB01000008.1_34	92.114	0.0	sseL	VF0947	TTSS-2 secreted effectors	Effector delivery system	VFC0086		(sseL) type III secretion system effector SseL, deubiquitinase [TTSS-2 secreted effectors (VF0947) - Effector delivery system (VFC0086)] [Salmonella enterica subsp. enterica serovar Typhimurium str. LT2]	Salmonella enterica (serovar typhimurium)
LAZB01000008.1_143	72.115	2.8E-173	pla	VF0139	Pla	Exoenzyme	VFC0251	Belongs to the family of OM proteases/adhesins known as omptins that share high sequence identity but differ in biological function; Omptins appear to constitute a unique class of proteases. Other omptin family outer membrane proteases include PgtE from S. enterica, OmpT and OmpR from E. coli, and SopA/IcsP from S. flexneri. Their catalytic residues are conserved. They require the presence of rough LPS for enzymatic activity and are inhibited by the O-antigen chains present in smooth LPS; unique to Y. pestis encoded by the pPCP1 plasmid not present in the enteropathogenic yersiniae Y. pseudotuberculosis and Y. enterocolitica	(pla) plasminogen activator protease precursor [Pla (VF0139) - Exoenzyme (VFC0251)] [Yersinia pestis CO92]	Yersinia pestis
LAZB01000008.1_288	69.892	0.0	rfaE	VF0044	LOS	Immune modulation	VFC0258	Lic1A (phosphorylcholine (ChoP) kinase) 5'-CAAT-3' within the 5'-end of its coding sequence; lic2A, also referred to as lexA, variation in the number of 5'-CAAT-3' repeats has been shown to correlate directly with phase variation of the Gal-alpha(1-4)beta-Gal LPS structure; But lgtC (glycosyltransferase), another phase-variable gene, ultimately dictates whether this structure is synthesized. lic3A encode a sialyl transferase which directs the substitution of LPS with sialic acid.	(rfaE) ADP-heptose synthase [LOS (VF0044) - Immune modulation (VFC0258)] [Haemophilus influenzae Rd KW20]	Haemophilus influenzae
LAZB01000008.1_358	60.0	1.7E-71	hcp/tssD	VF0944	HSI-3	Effector delivery system	VFC0086	The expression of T6SSs in P. aeruginosa is regulated by the QS system. There are several QS systems in P. aeruginosa, two N-acyl-homoserine lactone based QS systems (las and rhl systems) and one quinolone PQS system (pqs). The expression of H1-T6SS is negatively regulated by both las and pqs QS systems, while the expression of H2- and H3-T6SS is positively regulated by las, rhl, and pqs	(hcp/tssD) Hcp family type VI secretion system effector [HSI-3 (VF0944) - Effector delivery system (VFC0086)] [Pseudomonas aeruginosa PAO1]	Pseudomonas aeruginosa

Host	Gene count
Homo sapiens	3
environmental samples	3