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蛋白质 N-糖基化、蛋白质折叠和蛋白质质量控制。

Protein N-glycosylation, protein folding, and protein quality control.

机构信息

Department of Integrated OMICs for Biomedical Sciences, WCU Program of Graduate School, Yonsei University, Seoul 120-749, Korea.

出版信息

Mol Cells. 2010 Dec;30(6):497-506. doi: 10.1007/s10059-010-0159-z. Epub 2010 Nov 26.

Abstract

Quality control of protein folding represents a fundamental cellular activity. Early steps of protein N-glycosylation involving the removal of three glucose and some specific mannose residues in the endoplasmic reticulum have been recognized as being of importance for protein quality control. Specific oligosaccharide structures resulting from the oligosaccharide processing may represent a glycocode promoting productive protein folding, whereas others may represent glyco-codes for routing not correctly folded proteins for dislocation from the endoplasmic reticulum to the cytosol and subsequent degradation. Although quality control of protein folding is essential for the proper functioning of cells, it is also the basis for protein folding disorders since the recognition and elimination of non-native conformers can result either in loss-of-function or pathological-gain-of-function. The machinery for protein folding control represents a prime example of an intricate interactome present in a single organelle, the endoplasmic reticulum. Here, current views of mechanisms for the recognition and retention leading to productive protein folding or the eventual elimination of misfolded glycoproteins in yeast and mammalian cells are reviewed.

摘要

蛋白质折叠的质量控制代表了一种基本的细胞活动。在内质网中,涉及到去除三个葡萄糖和一些特定甘露糖残基的早期蛋白质 N-糖基化步骤已被认为对蛋白质质量控制很重要。糖基化处理产生的特定寡糖结构可能代表促进蛋白质有效折叠的糖码,而其他结构可能代表糖码,用于将未正确折叠的蛋白质分拣到内质网到细胞质中,并随后进行降解。尽管蛋白质折叠的质量控制对于细胞的正常功能至关重要,但它也是蛋白质折叠障碍的基础,因为识别和消除非天然构象可能导致功能丧失或病理性获得功能。蛋白质折叠控制的机制是存在于单个细胞器内质网中的复杂相互作用组的一个主要范例。在此,综述了酵母和哺乳动物细胞中识别和保留导致蛋白质有效折叠或最终消除错误折叠糖蛋白的机制的最新观点。

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