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比较基因鉴定-58(CGI-58)的 N 端区域对于与脂滴的结合以及脂肪甘油三酯脂肪酶的激活是重要的。

The N-terminal region of comparative gene identification-58 (CGI-58) is important for lipid droplet binding and activation of adipose triglyceride lipase.

机构信息

Institute of Molecular Biosciences, University of Graz, Humboldtstrasse, A-8010 Graz, Austria.

出版信息

J Biol Chem. 2010 Apr 16;285(16):12289-98. doi: 10.1074/jbc.M109.064469. Epub 2010 Feb 17.

Abstract

In mammals, excess energy is stored in the form of triacylglycerol primarily in lipid droplets of white adipose tissue. The first step of lipolysis (i.e. the mobilization of fat stores) is catalyzed by adipose triglyceride lipase (ATGL). The enzymatic activity of ATGL is strongly enhanced by CGI-58 (comparative gene identification-58), and the loss of either ATGL or CGI-58 function causes systemic triglyceride accumulation in humans and mice. However, the mechanism by which CGI-58 stimulates ATGL activity is unknown. To gain insight into CGI-58 function using structural features of the protein, we generated a three-dimensional homology model based on sequence similarity with other proteins. Interestingly, the model of CGI-58 revealed that the N terminus forms an extension of the otherwise compact structure of the protein. This N-terminal region (amino acids 1-30) harbors a lipophilic tryptophan-rich stretch, which affects the localization of the protein. (1)H NMR experiments revealed strong interaction between the N-terminal peptide and dodecylphosphocholine micelles as a lipid droplet-mimicking system. A role for this N-terminal region of CGI-58 in lipid droplet binding was further strengthened by localization studies in cultured cells. Although wild-type CGI-58 localizes to the lipid droplet, the N-terminally truncated fragments of CGI-58 are dispersed in the cytoplasm. Moreover, CGI-58 lacking the N-terminal extension loses the ability to stimulate ATGL, implying that the ability of CGI-58 to activate ATGL is linked to correct localization. In summary, our study shows that the N-terminal, Trp-rich region of CGI-58 is essential for correct localization and ATGL-activating function of CGI-58.

摘要

在哺乳动物中,多余的能量以三酰基甘油的形式主要储存在白色脂肪组织的脂滴中。脂肪分解(即脂肪储存的动员)的第一步是由脂肪甘油三酯脂肪酶(ATGL)催化的。CGI-58(比较基因鉴定-58)强烈增强 ATGL 的酶活性,ATGL 或 CGI-58 功能的丧失会导致人和小鼠的全身甘油三酯积累。然而,CGI-58 刺激 ATGL 活性的机制尚不清楚。为了利用该蛋白的结构特征深入了解 CGI-58 的功能,我们根据与其他蛋白的序列相似性生成了一个三维同源模型。有趣的是,CGI-58 的模型表明其 N 端形成了该蛋白紧凑结构的延伸。该 N 端区域(氨基酸 1-30)含有富含疏水性色氨酸的延伸部分,影响蛋白的定位。(1)H NMR 实验显示,该 N 端肽与十二烷基磷酸胆碱胶束之间存在强烈的相互作用,胶束模拟了脂滴。进一步的细胞定位研究强化了 CGI-58 的该 N 端区域在脂滴结合中的作用。尽管野生型 CGI-58 定位于脂滴,但 CGI-58 的 N 端截断片段分散在细胞质中。此外,缺乏 N 端延伸的 CGI-58 失去了刺激 ATGL 的能力,这表明 CGI-58 激活 ATGL 的能力与其正确的定位有关。总之,我们的研究表明,CGI-58 的 N 端富含色氨酸的区域对于 CGI-58 的正确定位和激活 ATGL 的功能是必需的。

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