OMIX009203

1Summary
Title SR-A3 suppresses AKT activation to protect against MAFLD by inhibiting XIAP-mediated PTEN degradation
Description Scavenger receptor class A member 3 (SR-A3) is implicated in metabolic diseases; however, the relationship between SR-A3 and metabolic dysfunction-associated fatty liver disease (MAFLD) has not been documented. Here, we show that hepatic SR-A3 expression is significantly reduced in human and animal models in the context of MAFLD. Genetic inhibition of SR-A3 in hamsters elicits hyperlipidemia, hyperglycemia, insulin resistance, and hepatic steatosis under chow-diet condition, yet escalates in diet-induced MAFLD. Mechanistically, SR-A3 ablation enhances E3 ligase XIAP-mediated proteasomal ubiquitination of PTEN, leading to AKT hyperactivation. By contrast, hepatic overexpression of human SR-A3 is sufficient to attenuate metabolic disorders in WT hamsters fed a high-fat-high-cholesterol diet and ob/ob mice via suppressing the XIAP/PTEN/AKT axis. In parallel, pharmacological intervention by PTEN agonist oroxin B or lipid lowering agent ezetimibe differentially corrects MAFLD in hamsters.
Organism Mesocricetus auratus
Data Type Lipidome Data by Mass Spectrometry (MS)
Data Accessibility Open-access
BioProject PRJCA036601
Release Date 2025-02-26
Submitter Yiran Liu (2010305121@stu.pku.edu.cn)
Organization Peking University Health Science Center
Submission Date 2025-02-25
2Files & Download

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File ID File Title Number/Samples File Type File Size File Suffix Download
OMIX009203-01 Lipidomics data 24 Lipidome Data by Mass Spectrometry (MS) 344.3 KB xlsx
3Relevant Publications
Paper Title Journal Name Publish Time Accession Citing Type
SR-A3 suppresses AKT activation to protect against MAFLD by inhibiting XIAP-mediated PTEN degradation Nature Communications 2025-03 OMIX009203 Deposit

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