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LSDP5是一种在脂肪酸氧化组织中特异性表达的PAT蛋白。

LSDP5 is a PAT protein specifically expressed in fatty acid oxidizing tissues.

作者信息

Dalen Knut Tomas, Dahl Tuva, Holter Elin, Arntsen Borghild, Londos Constantine, Sztalryd Carole, Nebb Hilde I

机构信息

Department of Nutrition, Institute of Basic Medical Sciences, University of Oslo, P.O. Box 1046 Blindern, N-0316 Oslo, Norway.

出版信息

Biochim Biophys Acta. 2007 Feb;1771(2):210-27. doi: 10.1016/j.bbalip.2006.11.011. Epub 2006 Dec 8.

Abstract

The PAT family (originally named for Perilipin, ADFP and TIP47) now includes four members: Perilipins, ADFP, TIP47 and S3-12. Significant primary sequence homology and the ability to associate with lipid storage droplets (LSDs) are well conserved within this family and across species. In this study, we have characterized a novel PAT protein, lipid storage droplet protein 5 (LSDP5) of 463 residues. A detailed sequence analysis of all murine PAT proteins reveals that LSDP5, TIP47 and ADFP share the highest order of sequence similarity, whereas perilipin and S3-12 have more divergent carboxyl- and amino-termini, respectively. Ectopically-expressed YFP-LSDP5 or flag-LSDP5 fusion proteins associate with LSDs. In accord with recent published data for perilipin, forced expression of LSDP5 in CHO cells inhibits lipolysis of intracellular LSDs. The LSDP5 gene is primarily transcribed in cells that actively oxidize fatty acids, such as heart, red muscle and liver. Expression of LSDP5 is stimulated by ligand activation of peroxisomal proliferator-activated receptor alpha (PPARalpha), and significantly reduced in liver and heart in the absence of this transcription factor. PPARalpha is generally required for regulation of fatty acid metabolism during fasting, but fasting induces LSDP5 mRNA in liver even in the absence of PPARalpha.

摘要

PAT家族(最初因围脂滴蛋白、脂肪分化相关蛋白和TIP47而得名)现在包括四个成员:围脂滴蛋白、脂肪分化相关蛋白、TIP47和S3-12。该家族成员之间以及不同物种之间,其主要序列同源性以及与脂质储存滴(LSDs)结合的能力都得到了很好的保留。在本研究中,我们鉴定了一种新的PAT蛋白,即含有463个氨基酸残基的脂质储存滴蛋白5(LSDP5)。对所有小鼠PAT蛋白的详细序列分析表明,LSDP5、TIP47和脂肪分化相关蛋白具有最高程度的序列相似性,而围脂滴蛋白和S3-12分别在羧基末端和氨基末端有更多的差异。异位表达的黄色荧光蛋白-LSDP5或flag-LSDP5融合蛋白与LSDs结合。与最近发表的关于围脂滴蛋白的数据一致,在CHO细胞中强制表达LSDP5可抑制细胞内LSDs的脂解作用。LSDP5基因主要在积极氧化脂肪酸的细胞中转录,如心脏、红色肌肉和肝脏。LSDP5的表达受过氧化物酶体增殖物激活受体α(PPARα)配体激活的刺激,在缺乏该转录因子时,肝脏和心脏中的表达显著降低。PPARα通常是禁食期间脂肪酸代谢调节所必需的,但即使在没有PPARα的情况下,禁食也会诱导肝脏中LSDP5 mRNA的表达。

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