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Controlling deuterium isotope effects in comparative proteomics

机译:在比较蛋白质组学中控制氘同位素的作用

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This paper focuses on identifying structural features responsible for resolution of heavy isotope coded peptides during reversed-phase chromatography. This was achieved by using labeled coding agents that varied in structure, number of deuterium atoms, placement of deuterium in the coding agent, and the functional group targeted by the reagent. Six coding agents were examined. Deuterated versions of the coding agents studied included succinic anhydride-H-2(4), acetic acid 2,5-dioxopyrrolidin-1-yl ester-H-2(3), propionic acid 2,5-dioxopyrrolidin-1-yl ester-H-2(5), pentanoic acid 2,5-dioxopyrrolidin-1-yl ester-H-2(9), [3-(2,5-dioxopyrrolidin-1-yloxycarbonyl)-propyl]-trimethylammonium chloride-H-2(9), and the commercial ICAT-H-2(8) reagent. It was found that these labeling agents vary widely in both their absolute and relative contribution to the chromatographic isotope effect. Relative effects were evaluated by normalizing resolution for the number of deuterium atoms in the derivatized peptide. The single, most dominant effect was the placement of deuterium atoms relative to hydrophilic functional groups in the coding agent. It was concluded that the probability of a deuterium atom interacting with the stationary phase of a reversed-phase chromatography (RPC) column and impacting resolution is greatly diminished by placing it adjacent to a hydrophilic group, as explained by solvophobic theory. But peptide size and coding agent size were also seen to correlate inversely with the magnitude of the isotope effect. This effect was explained as being due to the relative size of the coding agent versus that of the coding agent-peptide conjugate. [References: 24]
机译:本文着重于鉴定在反相色谱过程中负责解析重同位素编码肽的结构特征。这是通过使用结构,氘原子数,氘在编码剂中的位置以及试剂靶向的官能团不同的标记编码剂来实现的。检查了六种编码剂。研究的氘代编码剂包括琥珀酸酐-H-2(4),乙酸2,5-二氧杂吡咯烷-1-基酯-H-2(3),丙酸2,5-二氧杂吡咯烷-1-基酯-H-2(5),戊酸2,5-二氧杂吡咯烷-1-基酯-H-2(9),[3-(2,5-二氧杂吡咯烷-1-基氧羰基)-丙基]-三甲基氯化铵-H -2(9)和市售ICAT-H-2(8)试剂。发现这些标记剂对色谱同位素效应的绝对贡献和相对贡献都相差很大。通过归一化分辨率对衍生肽中氘原子的数量评估相对效果。唯一,最主要的作用是氘原子相对于编码剂中亲水性官能团的位置。结论是,如疏溶剂理论所解释,氘原子与反相色谱(RPC)色谱柱的固定相相互作用并影响分离的可能性大大降低了,因为氘原子与亲水基团相邻。但是,还发现肽大小和编码剂大小与同位素效应的大小成反比。解释该效果是由于编码剂相对于编码剂-肽缀合物的相对大小。 [参考:24]

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