| Literature DB >> 33490072 |
Jian-Jun Lv1, Hao Wang1, Hong-Yong Cui1, Ze-Kun Liu1, Ren-Yu Zhang1, Meng Lu1, Can Li1, Yu-Le Yong1, Man Liu1, Hai Zhang1, Tian-Jiao Zhang1, Kun Zhang1,2, Gang Li1,3, Gang Nan1, Cong Zhang1, Shuang-Ping Guo4, Ling Wang5, Zhi-Nan Chen1, Huijie Bian1.
Abstract
The persistence of macrophage-derived foam cells in the artery wall fuels atherosclerosis development. However, the mechanism of foam cell formation regulation remains elusive. We are committed to determining the role that CD147 might play in macrophage foam cell formation during atherosclerosis. In this study, we found that CD147 expression was primarily increased in mouse and human atherosclerotic lesions that were rich in macrophages and could be upregulated by ox-LDL. High-throughput compound screening indicated that ox-LDL-induced CD147 upregulation in macrophages was achieved through PI3K/Akt/mTOR signaling. Genetic deletion of macrophage CD147 protected against foam cell formation by impeding cholesterol uptake, probably through the scavenger receptor CD36. The opposite effect was observed in primary macrophages isolated from macrophage-specific CD147-overexpressing mice. Moreover, bioinformatics results indicated that CD147 suppression might exert an atheroprotective effect via various processes, such as cholesterol biosynthetic and metabolic processes, LDL and plasma lipoprotein clearance, and decreased platelet aggregation and collagen degradation. Our findings identify CD147 as a potential target for prevention and treatment of atherosclerosis in the future.Entities:
Keywords: CD147; CD36; atherosclerosis; foam cell formation; macrophage
Year: 2021 PMID: 33490072 PMCID: PMC7820343 DOI: 10.3389/fcell.2020.609090
Source DB: PubMed Journal: Front Cell Dev Biol ISSN: 2296-634X