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人类补体成分C9的序列与拓扑结构

The sequence and topology of human complement component C9.

作者信息

Stanley K K, Kocher H P, Luzio J P, Jackson P, Tschopp J

出版信息

EMBO J. 1985 Feb;4(2):375-82. doi: 10.1002/j.1460-2075.1985.tb03639.x.

Abstract

A partial nucleotide sequence of human complement component C9 cDNA representing 94% of the coding region of the mature protein is presented. The amino acid sequence predicted from the open reading frame of this cDNA concurs with the amino acid sequence at the amino-terminal end of three proteolytic fragments of purified C9 protein. No long stretches of hydrophobic residues are present, even in the carboxy-terminal half of the molecule which reacts with lipid-soluble photoaffinity probes. Monoclonal antibody epitopes have been mapped by comparing overlapping fragments of C9 molecule to which the antibodies bind on Western blots. Several of these epitopes map to small regions containing other surface features (e.g., proteolytic cleavage sites and N-linked oligosaccharide). The amino-terminal half of C9 is rich in cysteine residues and contains a region with a high level of homology to the LDL receptor cysteine-rich domains. A model for C9 topology based on these findings is proposed.

摘要

本文呈现了人类补体成分C9 cDNA的部分核苷酸序列,该序列代表成熟蛋白编码区的94%。从该cDNA的开放阅读框预测的氨基酸序列与纯化的C9蛋白的三个蛋白水解片段的氨基末端的氨基酸序列一致。即使在与脂溶性光亲和探针反应的分子的羧基末端一半中,也不存在长的疏水残基片段。通过比较C9分子的重叠片段(这些片段在蛋白质印迹上与抗体结合)来绘制单克隆抗体表位图谱。其中几个表位定位于含有其他表面特征(如蛋白水解切割位点和N-连接寡糖)的小区域。C9的氨基末端一半富含半胱氨酸残基,并且包含一个与低密度脂蛋白(LDL)受体富含半胱氨酸结构域具有高度同源性的区域。基于这些发现,提出了C9拓扑结构模型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2f33/554196/d4d7dfc28759/emboj00267-0100-a.jpg

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