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紫外激光诱导肽向氧化基质的电子转移:MALDI 源内降解质谱法第一步的研究。

Ultraviolet-Laser-Induced Electron Transfer from Peptides to an Oxidizing Matrix: Study of the First Step of MALDI In-Source Decay Mass Spectrometry.

机构信息

National Institute of Advanced Industrial Science and Technology (AIST), Tsukuba, Ibaraki 305-8568, Japan.

出版信息

J Am Soc Mass Spectrom. 2020 Sep 2;31(9):1918-1926. doi: 10.1021/jasms.0c00186. Epub 2020 Aug 4.

DOI:10.1021/jasms.0c00186
PMID:32687357
Abstract

Although the N-H bond in peptide backbones is stronger than the C-H bond, hydrogen abstraction from the amide nitrogen is considered to be the initial step in the C-C bond cleavage of peptide backbones by matrix-assisted laser desorption/ionization in-source decay (MALDI-ISD) when using an oxidizing matrix. MALDI-ISD induces C-C bond cleavage in most amino acid residues, whereas the N-terminal sides of proline (Pro) residues preferentially undergo peptide bond cleavage, which cannot be explained by the previously proposed mechanism involving hydrogen abstraction from peptides. To explain the whole MALDI-ISD process, electron abstraction from peptides by the oxidizing matrix is proposed as the initial step in the MALDI-ISD process. The electron abstraction occurs from either nitrogen or oxygen in the peptide backbone and induces the cleavage of both C-C and N-H bonds in most amino acid residues, except for those on the N-terminal sides of Pro residues. Electron abstraction from the Pro residues induces the cleavage of both peptide and C-C bonds, which is consistent with MALDI-ISD experimental results. The electron transfer from the peptide to the oxidizing matrix occurs simultaneously with the formation of matrix ions, which is considered to be the initial ion formation process in MALDI. The resultant peptide radical cation produces protonated and neutral molecules/radicals, which undergo subsequent ion-molecule reactions in the MALDI plume, finally yielding the ions that are observed in MALDI-ISD spectrum. As a result, the fragment ions formed by MALDI-ISD are observed as both positive and negative ions.

摘要

尽管肽骨架中的 N-H 键比 C-H 键强,但在使用氧化基质的基质辅助激光解吸/电离源内降解(MALDI-ISD)中,酰胺氮的氢提取被认为是肽骨架 C-C 键断裂的初始步骤。MALDI-ISD 诱导大多数氨基酸残基的 C-C 键断裂,而脯氨酸(Pro)残基的 N-末端优先发生肽键断裂,这不能用先前提出的涉及从肽中提取氢的机制来解释。为了解释整个 MALDI-ISD 过程,提出了氧化基质从肽中提取电子作为 MALDI-ISD 过程的初始步骤。电子从肽骨架中的氮或氧中提取,并诱导除 Pro 残基的 N-末端侧外的大多数氨基酸残基的 C-C 和 N-H 键断裂。从 Pro 残基中提取电子诱导肽和 C-C 键的断裂,这与 MALDI-ISD 实验结果一致。电子从肽转移到氧化基质与基质离子的形成同时发生,这被认为是 MALDI 中的初始离子形成过程。所得的肽自由基阳离子产生质子化和中性分子/自由基,它们在 MALDI 羽流中经历随后的离子-分子反应,最终生成在 MALDI-ISD 光谱中观察到的离子。因此,MALDI-ISD 形成的碎片离子既可以观察到正离子,也可以观察到负离子。

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