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嗜铬粒蛋白 A 作为将肽类激素分拣到分泌颗粒中的关键因素。

Chromogranin A as a crucial factor in the sorting of peptide hormones to secretory granules.

机构信息

Laboratory of Neuronal and Neuroendocrine Differentiation and Communication, INSERM U982, University of Rouen, Mont-St-Aignan Cedex, France.

出版信息

Cell Mol Neurobiol. 2010 Nov;30(8):1189-95. doi: 10.1007/s10571-010-9595-8. Epub 2010 Nov 3.

DOI:10.1007/s10571-010-9595-8
PMID:21046450
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11498877/
Abstract

Chromogranin A (CgA) is a soluble glycoprotein stored along with hormones and neuropeptides in secretory granules of endocrine cells. In the last four decades, intense efforts have been concentrated to characterize the structure and the biological function of CgA. Besides, CgA has been widely used as a diagnostic marker for tumors of endocrine origin, essential hypertension, various inflammatory diseases, and neurodegenerative disorders such as amyotrophic lateral sclerosis and Alzheimer's disease. CgA displays peculiar structural features, including numerous multibasic cleavage sites for prohormone convertases as well as a high proportion of acidic residues. Thus, it has been proposed that CgA represents a precursor of biologically active peptides, and a "granulogenic protein" that plays an important role as a chaperone for catecholamine storage in adrenal chromaffin cells. The widespread distribution of CgA throughout the neuroendocrine system prompted several groups to investigate the role of CgA in peptide hormone sorting to the regulated secretory pathway. This review summarizes the findings and theoretical concepts around the molecular machinery used by CgA to exert this putative intracellular function. Since CgA terminal regions exhibited strong sequence conservation through evolution, our work focused on the implication of these domains as potential functional determinants of CgA. Characterization of the molecular signals implicating CgA in the intracellular traffic of hormones represents a major biological issue that may contribute to unraveling the mechanisms defining the secretory competence of neuroendocrine cells.

摘要

嗜铬粒蛋白 A(CgA)是一种可溶性糖蛋白,与激素和神经肽一起储存在内分泌细胞的分泌颗粒中。在过去的四十年中,人们集中精力研究 CgA 的结构和生物学功能。此外,CgA 已被广泛用作内分泌来源肿瘤、原发性高血压、各种炎症性疾病以及神经退行性疾病(如肌萎缩侧索硬化症和阿尔茨海默病)的诊断标志物。CgA 具有独特的结构特征,包括许多用于激素原转化酶的多碱性裂解位点以及高比例的酸性残基。因此,有人提出 CgA 代表生物活性肽的前体,是一种“颗粒生成蛋白”,作为肾上腺嗜铬细胞儿茶酚胺储存的伴侣,发挥着重要作用。CgA 在神经内分泌系统中的广泛分布促使许多研究小组研究 CgA 在肽激素分拣到调节分泌途径中的作用。本文综述了围绕 CgA 发挥这种潜在细胞内功能所使用的分子机制的研究结果和理论概念。由于 CgA 末端区域在进化过程中表现出很强的序列保守性,我们的工作重点是这些结构域作为 CgA 潜在功能决定因素的意义。阐明涉及 CgA 激素细胞内运输的分子信号是一个重要的生物学问题,可能有助于揭示定义神经内分泌细胞分泌能力的机制。

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