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An acidic residue reactive and disulfide bond-containing cleavable crosslinker for probing protein 3D structures based on electrochemical mass spectrometry

机译:一种酸性残余物反应性和二硫键的可切割交联剂,用于探测基于电化学质谱法的蛋白质3D结构

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摘要

Cross-linking mass spectrometry (XL-MS) has attracted broad attention because of the capability to probe three-dimensional structure of proteins. Up to now, several amine-reactive cross-linkers have been developed for characterization of proteins and protein complexes. However, spatial information retrieved by XL-MS is still limited, partly because the strategies using an acidic residue reactive cross-linker have been rarely reported. In this paper, an acidic residue (e.g. aspartic acid, glutamic acid)-specific, disulfide bond-containing, cleavable cross-linker with a length of 13.1 angstrom, named 3,3'-dithiobis(propanoic dihydrazide), was presented for the first time. In addition, a novel approach using the cross-linker was proposed for unambiguous characterization of peptides and proteins with disulfide bonds. After cross-linked, the peptides could be electrochemically reduced, then characterized by high performance liquid chromatography mass spectrometry. For demonstration, the approach has been adopted to characterize the emideltide, insulin, and myoglobin, of which four pairs of intrachain cross-links have been successfully identified in myoglobin. The results showed that the cross-links displayed predictable fragmentation pattern upon collision induced dissociation (CID), thus admitting simplifying data analysis. In summary, this work introduces a novel type of cross-linker utilized for cross-linking and a new strategy to XL-MS technology for comprehensively understanding the three-dimensional structure of proteins.
机译:交联质谱(XL-MS)已引起因为探测蛋白质的三维结构的能力的广泛关注。截至目前,若干胺反应交联剂已被开发用于蛋白质和蛋白质复合物的表征。然而,通过XL-MS检索空间信息仍然有限,部分原因是由于使用酸性残基反应性交联剂的策略已经报道很少。在本文中,酸性残基(例如天冬氨酸,谷氨酸)特异性,二硫化键的,可裂解交联剂13.1埃的长度,名为3,3'-二硫代双(丙酸二酰肼),提出了第一次。此外,使用交联剂的新颖方法提出了肽和蛋白质与二硫键的明确的表征。后交联的,所述肽可以被电化学还原,然后通过高效液相色谱质谱表征。为了演示,该方法已被采用来表征emideltide,胰岛素和肌红蛋白,这四对链内交联已经在肌红蛋白被成功鉴定。结果表明,该交联在碰撞诱导解离(CID)显示预测的断裂模式,从而承认简化数据分析。总之,这项工作引入了一种新型的用于交联和一个新的策略以XL-MS技术全面认识蛋白质的三维结构利用交联剂。

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