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核受体介导的脂肪组织中脂滴相关蛋白基因表达的调控

Nuclear receptor-mediated regulation of lipid droplet-associated protein gene expression in adipose tissue.

作者信息

Christian Mark

机构信息

Division of Metabolic and Vascular Health, Warwick Medical School, University of Warwick, Coventry CV4 7AL, UK.

出版信息

Horm Mol Biol Clin Investig. 2013 Aug;14(3):87-97. doi: 10.1515/hmbci-2013-0028.

DOI:10.1515/hmbci-2013-0028
PMID:25436723
Abstract

In adipose tissues, nuclear receptors (NRs) have important metabolic actions on cellular lipid-storing capacity through targeted gene regulation. Lipid droplets (LDs) are the organelles for intracellular triacylglycerol (TAG) storage and are present in all eukaryotic cells. They are small in most cells, but in white adipocytes, they can occupy 90% of the cytoplasm. LDs consist of a TAG core surrounded by a phospholipid monolayer and an array of associated proteins that determine size, stability, inter-droplet interaction, and lipid storage capacity. The genes that encode these proteins are more highly expressed in brown compared with white fat, correlating with the greater LD surface area in multilocular brown adipocytes. Gene expression profiling reveals that most NRs are present in adipose tissues, with some showing greater expression in brown compared with white fat, including peroxisome proliferator-activated receptor (PPAR) α, estrogen-related receptor α, and NURR1. NR signaling is important for the regulated expression of most genes that encode LD-associated proteins. For example, estradiol signals via estrogen receptor α to regulate the levels of PLIN1 and the lipase ATGL controlling LD size and total lipid accumulation. PPARγ is essential for adipocyte differentiation and function, and analysis of data obtained through chromatin immunoprecipitation followed by high-throughput DNA sequencing shows that it binds to the promoters of many genes encoding LD proteins in adipocytes. Of these genes, the greatest PPARγ binding was to regulatory regions for Plin1, Cidec, and G0s2. NRs represent an important target for controlling LD dynamics in diseases affected by altered fat storage encompassing obesity and lipodystrophy, which are an increasing health problem.

摘要

在脂肪组织中,核受体(NRs)通过靶向基因调控对细胞脂质储存能力具有重要的代谢作用。脂滴(LDs)是细胞内三酰甘油(TAG)储存的细胞器,存在于所有真核细胞中。它们在大多数细胞中较小,但在白色脂肪细胞中,它们可占据细胞质的90%。脂滴由一个TAG核心组成,周围是磷脂单层以及一系列相关蛋白质,这些蛋白质决定了脂滴的大小、稳定性、脂滴间相互作用和脂质储存能力。与白色脂肪相比,编码这些蛋白质的基因在棕色脂肪中表达更高,这与多泡棕色脂肪细胞中更大的脂滴表面积相关。基因表达谱分析表明,大多数核受体存在于脂肪组织中,其中一些在棕色脂肪中的表达高于白色脂肪,包括过氧化物酶体增殖物激活受体(PPAR)α、雌激素相关受体α和NURR1。核受体信号传导对于大多数编码与脂滴相关蛋白质的基因的调控表达很重要。例如,雌二醇通过雌激素受体α发出信号,调节PLIN1和控制脂滴大小及总脂质积累的脂肪酶ATGL的水平。PPARγ对脂肪细胞的分化和功能至关重要,通过染色质免疫沉淀后进行高通量DNA测序获得的数据分析表明,它与脂肪细胞中许多编码脂滴蛋白的基因的启动子结合。在这些基因中,PPARγ结合最多的是Plin1、Cidec和G0s2的调控区域。核受体是控制受脂肪储存改变影响的疾病(包括肥胖症和脂肪营养不良,这是一个日益严重的健康问题)中脂滴动态的重要靶点。

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