NAFLDkb: a knowledge base and platform for drug development against non-alcoholic fatty liver disease

Research Article Details

Article ID:	A14234
PMID:	29512720
Source:	Mol Med Rep
Title:	Alogliptin alleviates hepatic steatosis in a mouse model of nonalcoholic fatty liver disease by promoting CPT1a expression via Thr172 phosphorylation of AMPKα in the liver.
Abstract:	Pioglitazone (PIO) has been reported to be effective for nonalcoholic fatty liver disease (NAFLD) and alogliptin (ALO) may have efficacy against NAFLD progression in patients with type 2 diabetes mellitus (T2DM). The present study examined the effectiveness of ALO in a rodent model of NAFLD and diabetes mellitus. KK‑Ay mice were used to produce an NAFLD model via administration of a choline‑deficient (CD) diet. To examine the effects of alogliptin, KK‑Ay mice were provided with a CD diet with 0.03% ALO and/or 0.02% PIO orally for 8 weeks. Biochemical parameters, pathological alterations and hepatic mRNA levels associated with fatty acid metabolism were assessed. Severe hepatic steatosis was observed in KK‑Ay mice fed with a CD diet, which was alleviated by the administration of ALO and/or PIO. ALO administration increased the hepatic carnitine palmitoyltransferase 1a (CPT1a) mRNA expression level and enhanced the Thr172 phosphorylation of AMP‑activated protein kinase α (AMPKα) in the liver. PIO administration tended to decrease the hepatic fatty acid synthase mRNA expression level and increase the serum adiponectin level. Homeostasis model of assessment‑insulin resistance values tended to improve with ALO and PIO administration. ALO and PIO alleviated hepatic steatosis in KK‑Ay mice fed with a CD diet. ALO increased hepatic mRNA expression levels associated with fatty acid oxidation. In addition, the results of the present study suggested that ALO promotes CPT1a expression via Thr172 phosphorylation of AMPKα.
DOI:	10.3892/mmr.2018.8673

Knowledge Graph
Associated Data

Strategy ID	Therapy Strategy	Synonyms	Therapy Targets	Therapy Drugs
S01	Improve insulin resistance	insulin sensitizer; insulin resistance; glucose tolerance	Biguanide: increases 5-AMP activated protein kinase signaling; SGLT-2 inhibitor; Thiazalidinedione: selective PPAR-γ agonists; GLP-1 agonist	Metformin; Empagliflozin; Canagliflozin; Rosiglitazone; Pioglitazone; Liraglutide	Details

Target ID	Target Name	GENE	Action	Class	UniProtKB ID	Entry Name
T01	5'-AMP-activated protein kinase subunit beta-1	PRKAB1	activator	Kinase	Q9Y478	AAKB1_HUMAN	Details
T10	Caspase-1	CASP1	inhibitor	Enzyme	P29466	CASP1_HUMAN	Details
T26	Thyroid hormone receptor beta	THRB	agonist	Nuclear hormone receptor	P10828	THB_HUMAN	Details
T20	Fatty acid synthase	FASN	inhibitor	Enzyme	P49327	FAS_HUMAN	Details

Diseases ID	DO ID	Disease Name	Definition	Class
I05	9352	Type 2 diabetes mellitus	A diabetes that is characterized by chronic hyperglycaemia with disturbances of carbohydrate, fat and protein metabolism resulting from defects in insulin secretion, insulin action, or both. A diabetes mellitus that is characterized by high blood sugar, insulin resistance, and relative lack of insulin. http://en.wikipedia.org/wiki/Diabetes, http://en.wikipedia.org/wiki/Diabetes_mellitus_type_2	disease of metabolism/inherited metabolic disorder/ carbohydrate metabolic disorder/glucose metabolism disease/diabetes/ diabetes mellitus	Details

Drug ID	Drug Name	Type	DrugBank ID	Targets	Category	Latest Progress
D328	Serine	Chemical drug	DB00133	SRR	Improve insulin resistance	Under clinical trials	Details
D201	L-Carnitine	Supplement	DB00583	SLC22A4; SLC22A5; CRAT; MPO	--	Under clinical trials	Details
D075	Choline	Supplement	DB00122	PLD2 product of; PLD1 product of	--	Under clinical trials	Details
D275	Pioglitazone	Chemical drug	DB01132	PPARG agonist	Improve insulin resistance	Advanced in clinical trials	Details
D182	Insulin	Biological drug	DB00030	INSR agonist; CPE modulator&product of	--	Under clinical trials	Details
D062	Carnitine complex	Supplement	DB00583	SLC22A4; SLC22A5; CRAT; MPO	--	Under clinical trials	Details