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人载脂蛋白 E2 异构体在脂肪细胞中的表达:改变了细胞加工过程,损害了脂肪细胞的脂生成。

Expression of the human apoE2 isoform in adipocytes: altered cellular processing and impaired adipocyte lipogenesis.

机构信息

Department of Medicine, University of Illinois at Chicago, Chicago, IL, USA.

出版信息

J Lipid Res. 2011 Sep;52(9):1733-41. doi: 10.1194/jlr.M017160. Epub 2011 Jul 8.

DOI:10.1194/jlr.M017160
PMID:21743035
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3151693/
Abstract

Expression of apoE in adipocytes has been shown to have an important role in modulating adipocyte triglyceride (TG) metabolism and gene expression that is independent of circulating and extracellular apoE. The impact of adipocyte expression of common human apoE isoforms was evaluated using adipocytes harvested from human apoE2, -3, and -4 knock-in mice. Expression of the apoE2 isoform was associated with an increase in adipocyte apoE gene expression and apoE synthesis. Newly synthesized apoE2 was unstable in adipocytes and demonstrated increased degradation and decreased secretion. ApoE2-expressing mice were hyperlipidemic, and had increased size of gonadal fat pads and of adipocytes, compared with apoE3 mice. In isolated cells, however, expression of the apoE2 isoform produced defective lipogenesis and increased TG hydrolysis. Incubation of adipose tissue with apoE3-containing TG-rich lipoproteins resulted in a significant increase in TG in adipose tissue from apoE3 and -E4 mice, but not apoE2 mice. Reduced capacity to internalize FFA as lipogenic substrate contributed to defective lipogenesis. Newly synthesized apoE2 is unstable in adipocytes and results in decreased adipocyte TG synthesis and defective FA uptake. These changes recapitulate those observed in apoE knockout adipocytes and have implications for understanding metabolic disturbances in humans expressing the E2 isoform.

摘要

脂肪细胞中载脂蛋白 E(apoE)的表达被证明在调节脂肪细胞三酰甘油(TG)代谢和基因表达方面具有重要作用,这种作用独立于循环和细胞外 apoE。本研究使用来自人 apoE2、-3 和 -4 基因敲入小鼠的脂肪细胞,评估了常见人类 apoE 同工型在脂肪细胞中的表达的影响。apoE2 同工型的表达与脂肪细胞 apoE 基因表达和 apoE 合成的增加有关。apoE2 在脂肪细胞中不稳定,表现为降解增加和分泌减少。与 apoE3 小鼠相比,apoE2 表达小鼠表现为血脂异常,且生殖腺脂肪垫和脂肪细胞的大小增加。然而,在分离的细胞中,apoE2 同工型的表达导致脂肪生成缺陷和 TG 水解增加。用含有 apoE3 的富含 TG 的脂蛋白孵育脂肪组织导致 apoE3 和 -E4 小鼠而不是 apoE2 小鼠的脂肪组织中 TG 显著增加。作为脂肪生成底物的 FFA 内化能力降低导致脂肪生成缺陷。新合成的 apoE2 在脂肪细胞中不稳定,导致脂肪细胞 TG 合成减少和 FA 摄取缺陷。这些变化再现了在 apoE 敲除脂肪细胞中观察到的变化,并对理解表达 E2 同工型的人类的代谢紊乱具有重要意义。

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