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从人胎盘中获得的一种独特胶原片段(内膜胶原)的结构多样性和结构域组成

Structural diversity and domain composition of a unique collagenous fragment (intima collagen) obtained from human placenta.

作者信息

Odermatt E, Risteli J, van Delden V, Timpl R

出版信息

Biochem J. 1983 May 1;211(2):295-302. doi: 10.1042/bj2110295.

Abstract

Intima collagen was obtained from pepsin digests of human placenta in two forms, which differ to some extent in the size of their constituent polypeptide chains (Mr 50 000-70 000). These chains are connected by disulphide bonds to large aggregates. The aggregates are arranged in a triple-helical conformation with a remarkably high thermal stability (Tm 41-62 degrees C) and are resistant to further proteolytic digestion. Reduction of as little as 5% of the disulphide bonds produces mainly monomeric triple helices (Mr about 160 000) with Tm 32 degrees C. Partially reduced material can be separated into triple-helical and non-collagenous domains by proteolysis. Pepsin releases a collagenous component with chains of Mr 38 000. Bacterial collagenase liberates two non-collagenous segments (Mr 15 000-30 000) rich in cystine. Treatment with collagenase before reduction separates intima collagen into a large fragment composed of collagenous (Tm 41 degrees C) and non-collagenous structures and a single non-collagenous segment. The data support the electron-microscopical model of intima collagen [Furthmayr, Wiedemann, Timpl, Odermatt & Engel (1983) Biochem. J. 211, 303-311], indicating that the basic unit of the fragment consists of a continuous triple helix joining two globular domains.

摘要

内膜胶原蛋白是从人胎盘的胃蛋白酶消化物中以两种形式获得的,它们组成多肽链的大小(分子量50000 - 70000)在一定程度上有所不同。这些链通过二硫键连接成大的聚集体。聚集体以三螺旋构象排列,具有非常高的热稳定性(熔点41 - 62℃),并且对进一步的蛋白水解消化具有抗性。仅还原5%的二硫键就主要产生单体三螺旋(分子量约160000),熔点为32℃。部分还原的物质可以通过蛋白水解分离为三螺旋和非胶原结构域。胃蛋白酶释放出分子量为38000的链的胶原成分。细菌胶原酶释放出两个富含胱氨酸的非胶原片段(分子量15000 - 30000)。在还原前用胶原酶处理可将内膜胶原蛋白分离成一个由胶原(熔点41℃)和非胶原结构组成的大片段以及一个单一的非胶原片段。这些数据支持内膜胶原蛋白的电子显微镜模型[Furthmayr、Wiedemann、Timpl、Odermatt和Engel(1983年)《生物化学杂志》211卷,303 - 311页],表明该片段的基本单位由连接两个球状结构域的连续三螺旋组成。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2af9/1154359/803b4ab8acfe/biochemj00353-0026-a.jpg

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