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表面活性蛋白C的生物合成及其在构象性肺病中的新作用。

Surfactant protein C biosynthesis and its emerging role in conformational lung disease.

作者信息

Beers Michael F, Mulugeta Surafel

机构信息

Pulmonary and Critical Care Division, Department of Medicine, University of Pennsylvania School of Medicine, Philadelphia, Pennsylvania 19104-6061, USA.

出版信息

Annu Rev Physiol. 2005;67:663-96. doi: 10.1146/annurev.physiol.67.040403.101937.

Abstract

Surfactant protein C (SP-C) is a hydrophobic 35-amino acid peptide that co-isolates with the phospholipid fraction of lung surfactant. SP-C represents a structurally and functionally challenging protein for the alveolar type 2 cell, which must synthesize, traffic, and process a 191-197-amino acid precursor protein through the regulated secretory pathway. The current understanding of SP-C biosynthesis considers the SP-C proprotein (proSP-C) as a hybrid molecule that incorporates structural and functional features of both bitopic integral membrane proteins and more classically recognized luminal propeptide hormones, which are subject to post-translational processing and regulated exocytosis. Adding to the importance of a detailed understanding of SP-C biosynthesis has been the recent association of mutations in the proSP-C sequence with chronic interstitial pneumonias in children and adults. Many of these mutations involve either missense or deletion mutations located in a region of the proSP-C molecule that has structural homology to the BRI family of proteins linked to inherited degenerative dementias. This review examines the current state of SP-C biosynthesis with a focus on recent developments related to molecular and cellular mechanisms implicated in the emerging role of SP-C mutations in the pathophysiology of diffuse parenchymal lung disease.

摘要

表面活性蛋白C(SP-C)是一种由35个氨基酸组成的疏水性肽,它与肺表面活性物质的磷脂部分共同分离。对于II型肺泡细胞而言,SP-C是一种在结构和功能上具有挑战性的蛋白质,该细胞必须通过调节性分泌途径合成、运输和加工一种由191 - 197个氨基酸组成的前体蛋白。目前对SP-C生物合成的理解认为,SP-C前体蛋白(proSP-C)是一种混合分子,它兼具双位整合膜蛋白以及更典型的腔内前肽激素的结构和功能特征,这些都要经过翻译后加工和调节性胞吐作用。近期proSP-C序列中的突变与儿童和成人的慢性间质性肺炎相关联,这使得详细了解SP-C生物合成的重要性进一步增加。其中许多突变涉及位于proSP-C分子中与遗传性退行性痴呆相关的BRI蛋白家族具有结构同源性的区域的错义或缺失突变。本综述探讨了SP-C生物合成的现状,重点关注与SP-C突变在弥漫性实质性肺疾病病理生理学中的新作用相关的分子和细胞机制的最新进展。

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