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首页> 外文期刊>Journal of the American Society for Mass Spectrometry >Imidate-Based Cross-Linkers for Structural Proteomics: Increased Charge of Protein and Peptide Ions and CID and ECD Fragmentation Studies
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Imidate-Based Cross-Linkers for Structural Proteomics: Increased Charge of Protein and Peptide Ions and CID and ECD Fragmentation Studies

机译:基于氨基甲酸酯的结构蛋白质组学交联剂:蛋白质和多肽离子电荷增加以及CID和ECD片段化研究

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摘要

Chemical cross-linking is an attractive low-resolution technique for structural studies of protein complexes. Distance constraints obtained from crosslinked peptides identified by mass spectrometry (MS) are used to construct and validate protein models. Amidinating cross-linkers such as diethyl suberthioimidate (DEST) have been used successfully in chemical cross-linking experiments. In this work, the application of a commercial diimidate cross-linking reagent, dimethyl suberimidate (DMS), was evaluated with model peptides and proteins. The peptides were designed with acetylated N-termini followed by random sequences containing two Lys residues separated by an Arg residue. After cross-linking reactions, intra- and intermolecular cross-linked species were submitted to CID and ECD dissociations to study their fragmentation features in the gas phase. Fragmentation of intramolecular peptides by collision induced dissociation (CID) demonstrates a unique two-step fragmentation pathway involving formation of a ketimine as intermediate. Electron capture and electron transfer dissociation (ECD and ETD) experiments demonstrated that the cyclic moiety is not dissociated. Intermolecular species demonstrated previously described fragmentation behavior in both CID and ECD experiments. The charge state distributions (CSD) obtained after reaction with DMS were compared with those obtained with disuccinimidyl suberate (DSS). CSDs for peptides and proteins were increased after their reaction with DMS, owing to the higher basicity of DMS modified species. These features were also observed in LC-MS experiments with bovine carbonic anhydrase II (BCA) after crosslinking with DMS and tryptic proteolysis. Cross-linked peptides derived from this protein were identified at high confidence and those species were in agreement with the crystal structure of BCA.
机译:化学交联是用于蛋白质复合物结构研究的一种有吸引力的低分辨率技术。从质谱(MS)鉴定的交联肽获得的距离限制可用于构建和验证蛋白质模型。酰胺化交联剂,如亚硫代次亚氨酸二乙酯(DEST)已成功用于化学交联实验中。在这项工作中,使用模型肽和蛋白质评估了商业化的二亚氨酸酯交联剂,亚甲基二亚磺酸酯(DMS)的应用。用乙酰化的N-末端设计肽,然后随机序列包含两个被Arg残基分隔的Lys残基。交联反应后,将分子内和分子间的交联物种进行CID和ECD解离,以研究其在气相中的破碎特征。通过碰撞诱导解离(CID)的分子内肽片段化显示出独特的两步片段化途径,其中涉及酮亚胺的形成。电子俘获和电子转移解离(ECD和ETD)实验表明,环状部分未解离。分子间物质在CID和ECD实验中均证明了先前描述的断裂行为。将与DMS反应后获得的电荷状态分布(CSD)与用辛二酸二琥珀酰亚胺酯(DSS)获得的电荷状态分布进行比较。与DMS反应后,由于DMS修饰物种的碱性较高,因此肽和蛋白质的CSD增加。在与DMS交联和胰蛋白酶解后,用牛碳酸酐酶II(BCA)进行的LC-MS实验中也观察到了这些特征。高度可靠地鉴定了衍生自该蛋白质的交联肽,这些物种与BCA的晶体结构一致。

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