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首页> 外文期刊>Journal of mass spectrometry: JMS >Structure characterization of lipocyclopeptide antibiotics, aspartocins A, B C, by ESI-MSMS and ESI-nozzle-skimmer-MSMS
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Structure characterization of lipocyclopeptide antibiotics, aspartocins A, B C, by ESI-MSMS and ESI-nozzle-skimmer-MSMS

机译:ESI-MSMS和ESI-喷嘴-撇油器-MSMS对脂环肽抗生素,天冬氨酸A,B C的结构表征

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Three lipocyclopeptide antibiotics, aspartocins A (1), B (2), and C (3), were obtained from the aspartocin complex by HPLC separation methodology. Their structures were elucidated using previously published chemical degradation results coupled with spectroscopic studies including ESI-MS, ESI-Nozzle Skimmer-MSMS and NMR. All three aspartocin compounds share the same cyclic decapeptide core of cyclo [Dab2 (Asp 1-FA)-Pip3-MeAsp4-Asp5-Gly6-Asp7-Gly8-Dab9-Val10-Pro11]. They differ only in the fatty acid side chain moiety (FA) corresponding to (Z)-13-methyltetradec-3-ene-carbonyl, (+,Z)-12-methyltetradec-3-ene-carbonyl and (Z)-12-methyltridec-3-ene-carbonyl for aspartocins A (1), B (2), and C (3), respectively. All of the sequence ions were observed by ESI-MSMS of the doubly charged parent ions. However, a number of the sequence ions observed were of low abundance. To fully sequence the lipocyclopeptide antibiotic structures, these low abundance sequence ions together with complementary sequence ions were confirmed by ESI-Nozzle-Skimmer-MSMS of the singly charged linear peptide parent fragment ions H-Asp5-Gly6-Asp7-Gly8-Dab9-Val10-Pro11-Dab2(1+)-Asp1-FA. Cyclization of the aspartocins was demonstrated to occur via the beta-amino group of Dab2 from ions of moderate intensity in the ESI-MSMS spectra. As the fatty acid moieties do not undergo internal fragmentations under the experimental ESI mass spectral conditions used, the 14 Da mass difference between the fatty acid moieties of aspartocins A (1) and B (2) versus aspartocin C (3) was used as an internal mass tag to differentiate fragment ions containing fatty acid moieties and those not containing the fatty acid moieties. The most numerous and abundant fragment ions observed in the tandem mass spectra are due to the cleavage of the tertiary nitrogen amide of the pipecolic acid residue-3 (16 fragment ions) and the proline residue-11 (7 fragmentions). In addition, the neutral loss of ethanimine from alpha,beta-diaminobutyric acid residue 9 was observed for the parent molecular ion and for 7 fragment ions
机译:通过HPLC分离方法从天冬氨酸复合物中获得了三种脂环肽抗生素,天冬氨酸A(1),B(2)和C(3)。使用先前发表的化学降解结果以及包括ESI-MS,ESI-Nozzle Skimmer-MSMS和NMR在内的光谱研究阐明了它们的结构。所有三种天冬氨酸化合物都具有相同的环[Dab2(Asp 1-FA)-Pip3-MeAsp4-Asp5-Gly6-Asp7-Gly8-Dab9-Val10-Pro11]环状十肽核心。它们仅在对应于(Z)-13-甲基十四碳烯-3-羰基,(+,Z)-12-甲基十四碳烯-3-羰基和(Z)-12的脂肪酸侧链部分(FA)上不同-甲基十三烷基-3-烯-羰基分别用于天冬氨酸A(1),B(2)和C(3)。通过双电荷母离子的ESI-MSMS观察到所有的序列离子。但是,观察到的许多序列离子的丰度较低。为了对脂环肽抗生素结构进行完全测序,这些低丰度序列离子以及互补序列离子通过单电荷线性肽母体片段离子H-Asp5-Gly6-Asp7-Gly8-Dab9-Val10的ESI-Nozzle-Skimmer-MSMS确认。 -Pro11-Dab2(1 +)-Asp1-FA。在ESI-MSMS光谱中,从中等强度的离子中,Dab2的β-氨基基团导致了天冬氨酸的环化。由于在使用的实验ESI质谱条件下脂肪酸部分不发生内部裂解,因此将天冬氨酸A(1)和B(2)与天冬氨酸C(3)的脂肪酸部分之间的14 Da质量差用作内部质量标签可区分包含脂肪酸基团的片段离子和不包含脂肪酸基团的片段离子。在串联质谱图中观察到的最多,最多的碎片离子是由于胡椒酸残基3(16个碎片离子)和脯氨酸残基11(7个碎片)的叔氮酰胺被裂解所致。此外,对于母体分子离子和7个碎片离子,观察到乙胺从α,β-二氨基丁酸9残基中性丢失

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