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膜联蛋白V一种新的高钙形式的晶体结构。

The crystal structure of a new high-calcium form of annexin V.

作者信息

Sopkova J, Renouard M, Lewit-Bentley A

机构信息

LURE, Centre Universitaire Paris-Sud, Orsay, France.

出版信息

J Mol Biol. 1993 Dec 5;234(3):816-25. doi: 10.1006/jmbi.1993.1627.

Abstract

Annexin V was crystallized in the presence of a high concentration of calcium and the structure refined at 1.9 A resolution. The crystals are triclinic (P1) with three molecules per asymmetric unit and pseudo-R3 symmetry, reflecting a tendency of annexin to form trimers. The overall structure of the protein is similar to that seen in other crystal forms. There are, however, significant changes in domain III, where a new calcium site is formed. The whole region surrounding this site is reorganized in our structure, rendering annexin V more symmetrical and more alike annexin I. The formation of the new calcium site causes the displacement of Trp187 from a buried to an exposed conformation, a change that has recently been demonstrated by fluorescence measurements. The affinity of the different potential calcium sites is modulated: there is no calcium bound in domains II and IV, while up to two secondary calcium ions sites (in domains I and III) can substitute, depending on the calcium concentration present. We suggest that annexin can act as a calcium buffer, binding or releasing calcium depending on its local concentration. Our results also show that annexin displays inherent mobility which, together with its capacity to modulate the calcium affinity of its sites, can be of importance for its function on the membrane surface.

摘要

膜联蛋白V在高浓度钙存在的情况下结晶,并在1.9埃分辨率下进行结构精修。晶体为三斜晶系(P1),每个不对称单元中有三个分子,具有假R3对称性,这反映了膜联蛋白形成三聚体的倾向。该蛋白质的整体结构与其他晶体形式中所见的结构相似。然而,结构域III有显著变化,其中形成了一个新的钙结合位点。在我们的结构中,围绕该位点的整个区域发生了重组,使膜联蛋白V更加对称,更类似于膜联蛋白I。新钙结合位点的形成导致色氨酸187从埋藏构象转变为暴露构象,最近的荧光测量已证实了这一变化。不同潜在钙结合位点的亲和力受到调节:结构域II和IV中没有结合钙,而根据存在的钙浓度,结构域I和III中最多可有两个二级钙离子位点可以替代。我们认为膜联蛋白可以作为一种钙缓冲剂,根据局部钙浓度结合或释放钙。我们的结果还表明,膜联蛋白具有内在的流动性,这与其调节其位点钙亲和力的能力一起,可能对其在膜表面的功能很重要。

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