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哺乳动物的NPC1和NPC2在肠道胆固醇吸收中起作用吗?

Do mammalian NPC1 and NPC2 play a role in intestinal cholesterol absorption?

作者信息

Dixit Sayali S, Sleat David E, Stock Ann M, Lobel Peter

机构信息

Center for Advanced Biotechnology and Medicine, 679 Hoes Lane, Piscataway, NJ 08854, USA.

出版信息

Biochem J. 2007 Nov 15;408(1):1-5. doi: 10.1042/BJ20071167.

Abstract

NPC1L1 (Niemann-Pick C1-like 1), the pharmacological target of the cholesterol-uptake inhibitor ezetimibe, is a transporter localized on the brush border of enterocytes. Although this protein plays a key role in intestinal uptake of sterols, multiple molecular events that underlie intestinal cholesterol absorption have not been fully characterized. Two proteins that might be involved in this process are NPC1 and NPC2 (Niemann-Pick disease type C proteins 1 and 2), which function in the endosomal/lysosomal cholesterol egress pathway and whose deficiency results in NPC (Niemann-Pick type C) disease. The involvement of these proteins in intestinal cholesterol absorption was examined in mutant mice lacking either NPC1 or NPC2. Our data indicate that deficiencies in either protein do not have an effect on cholesterol uptake or absorption. This contrasts with recent results obtained for the fruitfly Drosophila melanogaster, which indicate that a deficiency of NPC1 (dNPC1a being its Drosophila homologue) leads to activation of an NPC1L1 (Drosophila homologue dNPC1b)-independent cholesterol uptake pathway, underscoring fundamental differences in mammalian and non-mammalian cholesterol metabolism.

摘要

NPC1L1(尼曼-匹克C1样蛋白1)是胆固醇吸收抑制剂依泽替米贝的药理学靶点,是一种定位于肠上皮细胞刷状缘的转运蛋白。尽管该蛋白在肠道固醇吸收中起关键作用,但肠道胆固醇吸收所涉及的多个分子事件尚未完全明确。可能参与这一过程的两种蛋白是NPC1和NPC2(尼曼-匹克病C型蛋白1和2),它们在内体/溶酶体胆固醇释放途径中发挥作用,其缺乏会导致NPC(尼曼-匹克C型)病。在缺乏NPC1或NPC2的突变小鼠中研究了这些蛋白在肠道胆固醇吸收中的作用。我们的数据表明,这两种蛋白的缺乏对胆固醇摄取或吸收均无影响。这与最近在果蝇中获得的结果形成对比,果蝇的研究结果表明,NPC1(其果蝇同源物为dNPC1a)的缺乏会导致激活一条不依赖NPC1L1(果蝇同源物dNPC1b)的胆固醇摄取途径,这突出了哺乳动物和非哺乳动物胆固醇代谢的根本差异。

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Regulation of intestinal cholesterol absorption.肠道胆固醇吸收的调节
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The target of ezetimibe is Niemann-Pick C1-Like 1 (NPC1L1).依泽替米贝的作用靶点是尼曼-匹克C1样1蛋白(NPC1L1)。
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