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富含亮氨酸重复序列蛋白的结构多样性。

Structural diversity of leucine-rich repeat proteins.

作者信息

Kajava A V

机构信息

Swiss Institute for Experimental Cancer Research, Ch. des Boveresses 155, s/Lausanne, Epalinges, CH-1066, Switzerland.

出版信息

J Mol Biol. 1998 Apr 3;277(3):519-27. doi: 10.1006/jmbi.1998.1643.

Abstract

The superfamily of leucine-rich repeat proteins can be subdivided into at least six subfamilies, characterised by different lengths and consensus sequences of the repeats. It was proposed that the repeats from different subfamilies retain a similar superhelical fold, but differ in the three-dimensional structures of individual repeats. The sequence-structure relationship of three new subfamilies was examined by molecular modelling. I provide structural models for the repeats of all subfamilies. The models enable me to explain residue conservations within each subfamily. Furthermore, the difference in the packing explains why the repeats from different subfamilies never occur simultaneously in the same protein. Finally, these studies suggest different evolutionary origins for the different subfamilies. The approach used for the prediction of the leucine-rich repeat protein structures can be applied to other proteins containing internal repeats of about 20 to 30 residue in length.

摘要

富含亮氨酸重复序列的蛋白质超家族可至少细分为六个亚家族,其特征在于重复序列的长度和共有序列不同。有人提出,来自不同亚家族的重复序列保留了相似的超螺旋折叠,但各个重复序列的三维结构有所不同。通过分子建模研究了三个新亚家族的序列-结构关系。我提供了所有亚家族重复序列的结构模型。这些模型使我能够解释每个亚家族内的残基保守性。此外,堆积方式的差异解释了为什么来自不同亚家族的重复序列从未在同一蛋白质中同时出现。最后,这些研究表明不同亚家族有不同的进化起源。用于预测富含亮氨酸重复序列蛋白质结构的方法可应用于其他含有长度约为20至30个残基的内部重复序列的蛋白质。

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