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N-糖蛋白中 N-聚糖的合成、加工和功能。

Synthesis, Processing, and Function of N-Glycans in N-Glycoproteins.

机构信息

Department of Physiology, University of Kentucky College of Medicine, Lexington, KY, USA.

Veteran Affairs Medical Center, Lexington, KY, USA.

出版信息

Adv Neurobiol. 2023;29:65-93. doi: 10.1007/978-3-031-12390-0_3.

Abstract

Many membrane-resident and secreted proteins, including growth factors and their receptors are N-glycosylated. The initial N-glycan structure is synthesized in the endoplasmic reticulum (ER) as a branched structure on a lipid anchor (dolicholpyrophosphate) and then co-translationally, "en bloc" transferred and linked via N-acetylglucosamine to asparagine within a specific N-glycosylation acceptor sequence of the nascent recipient protein. In the ER and then the Golgi apparatus, the N-linked glycan structure is modified by hydrolytic removal of sugar residues ("trimming") followed by re-glycosylation with additional sugar residues ("processing") such as galactose, fucose or sialic acid to form complex N-glycoproteins. While the sequence of the reactions leading to biosynthesis, "en bloc" transfer and processing of N-glycans is well investigated, it is still not completely understood how N-glycans affect the biological fate and function of N-glycoproteins. This review will discuss the biology of N-glycoprotein synthesis, processing and function with specific reference to the physiology and pathophysiology of the immune and nervous system, as well as infectious diseases such as Covid-19.

摘要

许多膜结合蛋白和分泌蛋白,包括生长因子及其受体,都发生 N-糖基化。初始 N-聚糖结构在内质网(ER)中作为脂质锚(多萜醇焦磷酸)上的分支结构合成,然后在翻译过程中,“整体”转移并通过 N-乙酰葡萄糖胺与新生受体蛋白内特定 N-糖基化受体序列中的天冬酰胺连接。在 ER 中,然后在高尔基体中,N-连接的聚糖结构通过水解去除糖残基(“修剪”)进行修饰,然后通过添加额外的糖残基(“加工”),如半乳糖、岩藻糖或唾液酸,形成复杂的 N-糖蛋白。虽然导致生物合成、“整体”转移和 N-聚糖加工的反应序列已经得到很好的研究,但人们仍然不完全了解 N-聚糖如何影响 N-糖蛋白的生物学命运和功能。这篇综述将讨论 N-糖蛋白合成、加工和功能的生物学,特别参考免疫和神经系统的生理学和病理生理学,以及传染病如 Covid-19。

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