Persistent high glucose induced EPB41L4A-AS1 inhibits glucose uptake via GCN5 mediating crotonylation and acetylation of histones and non-histones.

Weijie LiaoNaihan XuHaowei ZhangWeifang LiaoYanzhi WangSongmao WangShikuan ZhangYuyang JiangWeidong XieYaou Zhang

Published in: Clinical and translational medicine (2022)

Our study first showed that the EPB41L4A-AS1/GCN5 complex repressed glucose uptake via targeting GLUT4/2 and TXNIP by regulating histone and nonhistone acetylation or crotonylation. Since a weaker glucose uptake ability is one of the major clinical features of T2DM, the inhibition of EPB41L4A-AS1 expression seems to be a potentially effective strategy for drug development in T2DM treatment.

Keyphrases

high glucose
endothelial cells
blood glucose
poor prognosis
dna methylation
histone deacetylase
type diabetes
diabetic rats
gene expression
cancer therapy
metabolic syndrome
blood pressure
long non coding rna
nlrp inflammasome
combination therapy
binding protein
insulin resistance
replacement therapy