通过表面诱导解吸高分辨质谱定位蛋白质复合物结合配体。
Localization of Protein Complex Bound Ligands by Surface-Induced Dissociation High-Resolution Mass Spectrometry.
机构信息
Department of Chemistry and Biochemistry , The Ohio State University , Columbus , Ohio 43210 , United States.
Protein Metrics Inc. , 20863 Stevens Creek Blvd., Suite 450 , Cupertino , California 95014 , United States.
出版信息
Anal Chem. 2018 Nov 6;90(21):12796-12801. doi: 10.1021/acs.analchem.8b03263. Epub 2018 Oct 26.
Abstract
Surface-induced dissociation (SID) is a powerful means of deciphering protein complex quaternary structures due to its capability of yielding dissociation products that reflect the native structures of protein complexes in solution. Here we explore the suitability of SID to locate the ligand binding sites in protein complexes. We studied C-reactive protein (CRP) pentamer, which contains a ligand binding site within each subunit, and cholera toxin B (CTB) pentamer, which contains a ligand binding site between each adjacent subunit. SID dissects ligand-bound CRP into subcomplexes with each subunit carrying predominantly one ligand. In contrast, SID of ligand-bound CTB results in the generation of subcomplexes with a ligand distribution reflective of two subunits contributing to each ligand binding site. SID thus has potential application in localizing sites of small ligand binding for multisubunit protein-ligand complexes.
摘要
表面诱导解离(SID)是一种强大的方法,可以解析蛋白质复合物的四级结构,因为它能够产生反映蛋白质复合物在溶液中天然结构的解离产物。在这里,我们探讨了 SID 用于定位蛋白质复合物中配体结合位点的适用性。我们研究了 C 反应蛋白(CRP)五聚体,其每个亚基内都含有一个配体结合位点,以及霍乱毒素 B(CTB)五聚体,其每个相邻亚基之间都含有一个配体结合位点。SID 将配体结合的 CRP 切割成亚基复合物,每个亚基主要携带一个配体。相比之下,配体结合的 CTB 的 SID 导致生成的亚基复合物具有配体分布,反映出两个亚基都参与每个配体结合位点。因此,SID 有可能应用于定位多亚基蛋白-配体复合物中小配体结合位点。
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