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在大氩簇离子轰击下的二次离子质谱中肽的解离模式。

Peptide dissociation patterns in secondary ion mass spectrometry under large argon cluster ion bombardment.

机构信息

Department of Physics and Research Center OPTIMAS, University of Kaiserslautern, Kaiserslautern, Germany.

出版信息

Rapid Commun Mass Spectrom. 2013 Jul 15;27(13):1490-6. doi: 10.1002/rcm.6599.

Abstract

RATIONALE

The analysis of organic and biological substances by secondary ion mass spectrometry (SIMS) has greatly benefited from the use of cluster ions as primary bombarding species. Thereby, depth profiling and three-dimensional (3D) imaging of such systems became feasible. Large Ar(n)(+) cluster ions may constitute a further improvement in this direction.

METHODS

To explore this option, large Ar(n)(+) cluster ions (with n ~1500 Ar atoms per cluster) were used to investigate the emission of positive secondary ions from two peptide specimens (angiotensin I and bradykinin) by orthogonal time-of-flight SIMS using bombarding energies 6, 10 and 14 keV.

RESULTS

For both peptides, the protonated molecular ion is observed in the mass spectra. In addition, distinct fragmentation patterns were observed; these indicate that fragment ions under Ar cluster irradiation form primarily via cleavage of bonds along the peptide backbone whereas the rapture of side chains occurs much less frequently. These features appear to be similar to low-energy collision-induced dissociation pathways.

CONCLUSIONS

Tentatively, these findings can then be ascribed to the concerted action of the large number of Ar atoms in the impact zone of cluster at the surface: these low-energy Ar species (with an average energy of few eV) may effect the cleavage of the peptide bonds and lead, eventually, to the emission of the fragment ions.

摘要

原理

利用二次离子质谱(SIMS)分析有机和生物物质,通过使用簇离子作为初级轰击物种,大大受益。由此,对这些系统进行深度剖析和三维(3D)成像成为可能。大的 Ar(n)(+)簇离子可能在此方向上构成进一步的改进。

方法

为了探索这种选择,使用大的 Ar(n)(+)簇离子(每个簇含有约 1500 个 Ar 原子),通过正交飞行时间 SIMS,用 6、10 和 14 keV 的轰击能量,研究了两种肽标本(血管紧张素 I 和缓激肽)中正二次离子的发射。

结果

对于两种肽,在质谱中都观察到了质子化的分子离子。此外,还观察到了明显的碎片化模式;这表明,在 Ar 簇辐照下形成的碎片离子主要是通过肽主链中键的断裂形成的,而侧链的断裂发生的频率要低得多。这些特征似乎类似于低能碰撞诱导解离途径。

结论

这些发现可能归因于簇在表面的冲击区中大量 Ar 原子的协同作用:这些低能 Ar 物种(平均能量为几个电子伏特)可能会影响肽键的断裂,并最终导致碎片离子的发射。

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