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MSn characterization of protonated cyclic peptides and metal complexes

机译:质子化环肽和金属络合物的MSn表征

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MSn experiments involving low energy collisionally activated dissociation (CAD) in a quadrupole ion trap were used to characterize the fragmentation of alkali, alkaline earth and transition metal complexes of five cyclic peptides, and the results were compared with those obtained for protonated cyclic peptides. Complexes with metal ions produced enhanced abundances of the most diagnostic fragments for elucidating the primary structures. For cyclosporin A, nickel and lithium complexes gave additional sequence information compared with the protonated peptide. For depsipeptides, sodium and lead complexes were superior to the protonated peptide or other metal complexes for sequencing residues, and CAD of the lead complexes led to preferential cleavage of two residues at a time. For cyclic lipopeptides, complexes with silver, nickel and strontium ions provided enhanced abundances of key fragment ions. (C) 2004 American Society for Mass Spectrometry.
机译:MSn实验涉及四极离子阱中的低能碰撞活化解离(CAD),用于表征五个环肽的碱,碱土金属和过渡金属配合物的断裂,并将结果与​​质子化环肽的结果进行比较。与金属离子的配合物可提高大多数诊断片段的丰度,从而阐明一级结构。对于环孢菌素A,与质子化肽相比,镍和锂复合物提供了更多的序列信息。对于十肽,钠和铅配合物在测序残基方面优于质子化肽或其他金属配合物,并且铅配合物的CAD可一次优先切割两个残基。对于环状脂肽,与银,镍和锶离子的配合物可增强关键片段离子的丰度。 (C)2004年美国质谱学会。

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