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化学交联和质谱作为一种低分辨率的蛋白质结构测定技术。

Chemical cross-linking and mass spectrometry as a low-resolution protein structure determination technique.

机构信息

Department of Medicinal Chemistry, University of Washington, Seattle, Washington 98195-7610, USA.

出版信息

Anal Chem. 2010 Apr 1;82(7):2636-42. doi: 10.1021/ac1000724.

Abstract

Protein complexes are the foundation of a majority of cellular processes. Although a large number of protein complexes have been identified through biochemical experiments, the precise molecular details and three-dimensional structures are available for only a small fraction. Chemical cross-linking coupled with mass spectrometry (CXMS) has gained popularity in recent years for characterization of inter- and intraprotein interactions in protein complexes. This perspective provides a comprehensive and critical overview of CXMS strategies employed for structural elucidation of protein complexes. We evaluate the challenges associated with CXMS techniques with special emphasis on data analysis. As sensitivity, mass resolution, mass accuracy and ease of use of mass spectrometers have improved, the complexity of processing and interpreting CXMS data has become the central problem to be addressed. We review here a number of computer programs available to address these problems.

摘要

蛋白质复合物是大多数细胞过程的基础。虽然已经通过生化实验鉴定了大量的蛋白质复合物,但只有一小部分具有精确的分子细节和三维结构。近年来,化学交联结合质谱(CXMS)在蛋白质复合物中蛋白质相互作用的表征方面越来越受欢迎。本综述全面而批判性地概述了用于蛋白质复合物结构阐明的 CXMS 策略。我们评估了与 CXMS 技术相关的挑战,特别强调了数据分析。随着质谱仪的灵敏度、质量分辨率、质量精度和易用性的提高,处理和解释 CXMS 数据的复杂性已成为需要解决的核心问题。我们在这里回顾了一些可用于解决这些问题的计算机程序。

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