Vascular Biology Group, Department of Biological and Biomedical Sciences, Glasgow Caledonian University, Glasgow G4 0BA, UK.
Clin Sci (Lond). 2010 Jun 22;119(7):265-72. doi: 10.1042/CS20100266.
Dysregulated macrophage cholesterol homoeostasis lies at the heart of early and developing atheroma, and removal of excess cholesterol from macrophage foam cells, by efficient transport mechanisms, is central to stabilization and regression of atherosclerotic lesions. The present study demonstrates that transient overexpression of STARD3 {START [StAR (steroidogenic acute regulatory protein)-related lipid transfer] domain 3; also known as MLN64 (metastatic lymph node 64)}, an endosomal cholesterol transporter and member of the 'START' family of lipid trafficking proteins, induces significant increases in macrophage ABCA1 (ATP-binding cassette transporter A1) mRNA and protein, enhances [(3)H]cholesterol efflux to apo (apolipoprotein) AI, and reduces biosynthesis of cholesterol, cholesteryl ester, fatty acids, triacylglycerol and phospholipids from [(14)C]acetate, compared with controls. Notably, overexpression of STARD3 prevents increases in cholesterol esterification in response to acetylated LDL (low-density lipoprotein), blocking cholesteryl ester deposition. Thus enhanced endosomal trafficking via STARD3 induces an anti-atherogenic macrophage lipid phenotype, positing a potentially therapeutic strategy.
巨噬细胞胆固醇稳态失调是动脉粥样硬化早期和进展的核心,通过有效的转运机制将巨噬细胞泡沫细胞中的胆固醇清除,对于动脉粥样硬化病变的稳定和消退至关重要。本研究表明,内体胆固醇转运蛋白和“START”家族脂质转运蛋白成员 STARD3(甾醇激活转录蛋白相关脂质转移域 3;也称为 MLN64(转移性淋巴结 64))的瞬时过表达可显著增加巨噬细胞 ABCA1(ATP 结合盒转运蛋白 A1)mRNA 和蛋白的表达,增强 [(3)H]胆固醇向载脂蛋白 AI 的流出,并减少 [(14)C]乙酰基从乙酸盐合成胆固醇、胆固醇酯、脂肪酸、三酰基甘油和磷脂,与对照组相比。值得注意的是,STARD3 的过表达可防止乙酰化 LDL(低密度脂蛋白)引起的胆固醇酯化增加,阻止胆固醇酯沉积。因此,通过 STARD3 增强内体转运可诱导抗动脉粥样硬化的巨噬细胞脂质表型,提出了一种潜在的治疗策略。
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