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蛋白质-蛋白质相互作用结构生物学中的连接子。

Linkers in the structural biology of protein-protein interactions.

机构信息

Department of Biological Sciences, National University of Singapore, Singapore 117543, Singapore.

出版信息

Protein Sci. 2013 Feb;22(2):153-67. doi: 10.1002/pro.2206. Epub 2013 Jan 8.


DOI:10.1002/pro.2206
PMID:23225024
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3588912/
Abstract

Linkers or spacers are short amino acid sequences created in nature to separate multiple domains in a single protein. Most of them are rigid and function to prohibit unwanted interactions between the discrete domains. However, Gly-rich linkers are flexible, connecting various domains in a single protein without interfering with the function of each domain. The advent of recombinant DNA technology made it possible to fuse two interacting partners with the introduction of artificial linkers. Often, independent proteins may not exist as stable or structured proteins until they interact with their binding partner, following which they gain stability and the essential structural elements. Gly-rich linkers have been proven useful for these types of unstable interactions, particularly where the interaction is weak and transient, by creating a covalent link between the proteins to form a stable protein-protein complex. Gly-rich linkers are also employed to form stable covalently linked dimers, and to connect two independent domains that create a ligand-binding site or recognition sequence. The lengths of linkers vary from 2 to 31 amino acids, optimized for each condition so that the linker does not impose any constraints on the conformation or interactions of the linked partners. Various structures of covalently linked protein complexes have been described using X-ray crystallography, nuclear magnetic resonance and cryo-electron microscopy techniques. In this review, we evaluate several structural studies where linkers have been used to improve protein quality, to produce stable protein-protein complexes, and to obtain protein dimers.

摘要

连接子或间隔子是在自然界中创建的短氨基酸序列,用于将单个蛋白质中的多个结构域分开。它们大多数是刚性的,其功能是防止离散结构域之间的不期望相互作用。然而,富含甘氨酸的连接子是灵活的,可在不干扰每个结构域功能的情况下连接单个蛋白质中的各种结构域。重组 DNA 技术的出现使得可以通过引入人工连接子将两个相互作用的伴侣融合在一起。通常,独立的蛋白质在与它们的结合伴侣相互作用之前可能不会作为稳定或结构化的蛋白质存在,之后它们获得稳定性和必需的结构元件。富含甘氨酸的连接子已被证明对这些类型的不稳定相互作用很有用,特别是在相互作用较弱且短暂的情况下,通过在蛋白质之间形成共价键来形成稳定的蛋白质-蛋白质复合物。富含甘氨酸的连接子还用于形成稳定的共价连接二聚体,并连接形成配体结合位点或识别序列的两个独立结构域。连接子的长度从 2 到 31 个氨基酸不等,针对每种情况进行了优化,以使连接子不会对连接伴侣的构象或相互作用施加任何限制。已经使用 X 射线晶体学、核磁共振和冷冻电子显微镜技术描述了各种共价连接的蛋白质复合物的结构。在这篇综述中,我们评估了几种使用连接子来提高蛋白质质量、产生稳定的蛋白质-蛋白质复合物和获得蛋白质二聚体的结构研究。

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