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Infrared Multiphoton Dissociation for Enhanced de Novo Sequence Interpretation of N-Terminal Sulfonated Peptides in a Quadrupole Ion Trap

机译:红外多光子解离用于增强四极杆离子阱中N末端磺化肽的从头序列解释

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Infrared multiphoton dissociation (IRMPD) of N-terminal sulfonated peptides improves de novo sequencing capabilities in a quadrupole ion trap mass spectrometer. Not only does IRMPD promote highly efficient dissociation of the N-terminal sulfonated peptides but also the entire series of y ions down to the y_(1) fragment may be detected due to alleviation of the low-mass cutoff problem associated with conventional collisional activated dissociation (CAD) methods in a quadrupole ion trap. Commercial de novo sequencing software was applied for the interpretation of CAD and IRMPD MS/MS spectra collected for seven unmodified peptides and the corresponding N-terminal sulfonated species. In most cases, the additional information obtained by N-terminal sulfonation in combination with IRMPD provided significant improvements in sequence identification. The software sequence tag results were combined with a commercial database searching algorithm to interpret sequence information of a tryptic digest on alpha-casein s1. Energy-variable CAD studies confirmed a 30-40percent reduction in the critical energies of the N-terminal sulfonated peptides relative to unmodified peptides. This reduction in dissociation energy facilitates IRMPD in a quadrupole ion trap.
机译:N末端磺化肽段的红外多光子解离(IRMPD)改善了四极杆离子阱质谱仪的从头测序功能。 IRMPD不仅可以促进N末端磺化肽的高效解离,而且由于减轻了与常规碰撞活化解离有关的低质量截止问题,可以检测到直至y_(1)片段的整个y离子序列。四极离子阱中的(CAD)方法。应用商用从头测序软件来解释收集的七个未修饰肽和相应的N端磺化物种的CAD和IRMPD MS / MS谱图。在大多数情况下,通过N末端磺化与IRMPD结合获得的其他信息可显着改善序列鉴定。将软件序列标签结果与商业数据库搜索算法组合,以解释α-酪蛋白s1上胰蛋白酶消化的序列信息。能量可变的CAD研究证实,与未修饰的肽相比,N末端磺化肽的临界能量降低了30-40%。解离能的这种降低促进了四极离子阱中的IRMPD。

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