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前蛋白转化酶枯草溶菌素1(PCSK1)的遗传与功能特性分析

Genetic and functional characterization of PCSK1.

作者信息

Choquet Hélène, Stijnen Pieter, Creemers John W M

机构信息

CNRS-8090-Institute of Biology, Pasteur Institute, Lille, France.

出版信息

Methods Mol Biol. 2011;768:247-53. doi: 10.1007/978-1-61779-204-5_13.

Abstract

PC1/3 is a neuroendocrine-specific member of the mammalian subtilisin-like proprotein convertase family. This seven-member family is involved in the endoproteolytic cleavage of a large number of precursor proteins including prohormones, proneuropeptides, zymogens, and proreceptors. PC1/3 is synthesized as a zymogen, proPC1/3, and its propeptide is rapidly and autocatalytically cleaved in the endoplasmic reticulum. The mature protein is sorted and stored in dense-core secretory vesicles, together with its substrates. Compound-inactivating mutations in the PCSK1 gene, which encodes PC1/3, cause monogenic obesity. Furthermore, the contribution of two common nonsynonymous variants in PCSK1 to polygenic obesity risk has recently been established. Additional rare variants have been identified in non-consanguineous extremely obese Europeans but functional characterization has not yet been described. Sequencing efforts of larger cohorts of obese patients might reveal more variants conferring risk of obesity.

摘要

PC1/3是哺乳动物枯草杆菌蛋白酶样前体蛋白转化酶家族中神经内分泌特异性成员。这个由七个成员组成的家族参与大量前体蛋白的内蛋白水解切割,包括激素原、神经肽原、酶原和前受体。PC1/3作为一种酶原即前PC1/3合成,其前肽在内质网中迅速进行自催化切割。成熟蛋白与其底物一起被分选并储存于致密核心分泌囊泡中。编码PC1/3的PCSK1基因中的复合失活突变会导致单基因肥胖。此外,最近已确定PCSK1中两个常见的非同义变体对多基因肥胖风险的影响。在非近亲的极度肥胖欧洲人中还鉴定出了其他罕见变体,但尚未对其进行功能表征。对更多肥胖患者队列进行测序可能会发现更多导致肥胖风险的变体。

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