Gene "SPAST"
Found 1 record
Gene information
Gene symbol:
SPAST
See related:
Ensembl: ENSG00000021574, Gene ID: 6683
Additive variants :
Detected
Genetic interaction partners
Confidence      Stringent (ε>0.16 or ε<-0.12)      Intermediate (-0.16≤ε≤-0.08 or 0.08≤ε≤0.16)      Lenient (|ε|<0.08)
Positive interactions
  • EEF1G 
  • UBE2F-SCLY 
  • PKLR 
  • EIF2B1 
  • UBE2V2 
  • SRXN1 
  • MAEA 
  • SMARCAD1 
  • RBBP5 
  • VAT1L 
  • POLI 
  • CSNK2B 
  • HIBCH 
  • FMO5 
  • RPS6 
  • RPS4X 
  • CWH43 
  • SLC11A2 
  • ZFP42 
  • TXNL1 
  • ATP1A1 
  • IMPACT 
  • USP17L30 
  • CTDSPL2 
  • TCF25 
  • EPS15 
  • ANKZF1 
  • FOXJ3 
  • PPP6C 
  • TRMT10B 
  • OMA1 
  • NKTR 
  • RPL13 
  • SCAP 
  • PPP2R5C 
  • ABCD3 
  • REXO5 
  • ACSF2 
  • PRKD1 
  • SDSL 
Negative interactions
  • BIN3 
  • CLIP1 
  • NAA30 
  • SIN3A 
  • XRN1 
  • THNSL1 
  • SMARCB1 
  • RPS10 
  • DNM1L 
  • ELOVL1 
  • ROMO1 
  • UBE4B 
  • GEN1 
  • EP400 
  • RAB24 
  • KIF2C 
  • PMS1 
  • ASF1A 
  • ZDHHC4 
  • CHPT1 
  • RPL35 
  • ACTR6 
  • LIPT1 
  • MSH2 
  • DPYSL2 
  • NAPEPLD 
  • WRN 
  • MAF1 
  • C2orf76 
  • ERN1 
  • ARL1 
  • CHTF18 
  • NTHL1 
  • ADHFE1 
  • GLRX3 
  • IDO1 
  • CLK2 
  • TOM1 
  • PELO 
  • COG6 
  • PAQR3 
  • PLD1 
  • PTPRN2 
  • HCFC2 
  • ETFA 
  • XRCC3 
  • ATP23 
  • SNAPC4 
  • TALDO1 
  • PICALM 
  • CPT2 
  • USP4 
  • UBXN7 
  • PAPSS1 
  • ELP3 
  • MOK 
  • POMT2 
  • VRK1 
  • RPEL1 
  • FOXJ3 
  • HAAO 
  • CCNA2 
  • SLC25A32 
  • TMEM165 
  • RPL27 
  • MUS81 
  • CYB5B 
Modifier statisitcs
Record:
Disorder:
Vriant:
Reference:
Effect type:
Expressivity(1)  
Modifier effect:
Altered phenotype(1)  
Detail:
  • Variant 1:
    SPAST:rs121908517
    Gene:
    SPAST
    Genomic location:
    dbSNP ID:
    rs121908517
    Target disease:
    Hereditary spastic paraplegia(DOID_2476)
    Effect type:
    Expressivity 
    Modifier effect:
    Altered phenotype 
    Evidence:
    Pedigree analysis 
    Effect:
    modify the HSP phenotype
    Reference:
    PMID15248095
    Title:
    Intragenic modifiers of hereditary spastic paraplegia due to spastin gene mutations
    Species studied:
    Human
    Abstract:
    Hereditary spastic paraplegia (HSP) is a genetically heterogeneous neurodegenerative disease characterized by wide variability in phenotypic expression, both within and among families. The most-common cause of autosomal dominant HSP is mutation of the gene encoding spastin, a protein of uncertain function. We report the existence of intragenic polymorphisms of spastin that modify the HSP phenotype. One (S44L) is a previously described recessively acting allele and the second is a novel allele affecting the adjacent amino acid residue (P45Q). In 4 HSP families in which either L44 or Q45 segregates independently of a missense or splicing mutation in the AAA domain of spastin, L44 and Q45 are each associated with a striking decrease in age at onset in the presence of the AAA domain mutations. Using a bioinformatics approach, we found that the highly conserved S44 is predicted to be phosphorylated by a number of family members of the proline-directed serine/threonine cyclin-dependent kinases (Cdks). Cdk1 and Cdk5 showed no kinase activity toward synthetic spastin peptide in an in vitro kinase assay, suggesting that this serine residue may be phosphorylated by a different Cdk. Our identification of S44L and P45Q as modifiers of the HSP phenotype suggests a role for spastin phosphorylation by Cdks in the neurodegeneration of the most-common form of HSP.