首页> 外文期刊>Molecular & cellular proteomics: MCP >An Improved Model for Prediction of Retention Times of Tryptic Peptides in Ion Pair Reversed-phase HPLC: Its Application to Protein Peptide Mapping by Off-Line HPLC-MALDI MS.
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An Improved Model for Prediction of Retention Times of Tryptic Peptides in Ion Pair Reversed-phase HPLC: Its Application to Protein Peptide Mapping by Off-Line HPLC-MALDI MS.

机译:胰蛋白酶肽在离子对反相HPLC中保留时间预测的改进模型:其在离线HPLC-MALDI MS进行蛋白质肽图分析中的应用。

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摘要

The proposed model is based on the measurement of the retention times of 346 tryptic peptides in the 560- to 4,000-Da mass range, derived from a mixture of 17 protein digests. These peptides were measured in HPLC-MALDI MS runs, with peptide identities confirmed by MS/MS. The model relies on summation of the retention coefficients of the individual amino acids, as in previous approaches, but additional terms are introduced that depend on the retention coefficients for amino acids at the N-terminal of the peptide. In the 17-protein mixture, optimization of two sets of coefficients, along with additional compensation for peptide length and hydrophobicity, yielded a linear dependence of retention time on hydrophobicity, with an R(2) value about 0.94. The predictive capability of the model was used to distinguish peptides with close m/z values and for detailed peptide mapping of selected proteins. Its applicability was tested on columns of different sizes, from nano- to narrow-bore, and for direct sample injection, or injection via a pre-column. It can be used for accurate prediction of retention times for tryptic peptides on reversed-phase (300-A pore size) columns of different sizes with a linear water-ACN gradient and with TFA as the ion-pairing modifier.
机译:所提出的模型基于对560到4,000 Da质量范围内346种胰蛋白酶肽的保留时间的测量,该肽来自17种蛋白质消化物的混合物。在HPLC-MALDI MS运行中测量这些肽,并通过MS / MS确认肽身份。与以前的方法一样,该模型依赖于各个氨基酸的保留系数的总和,但引入了其他术语,这些术语取决于肽N端氨基酸的保留系数。在17种蛋白质的混合物中,两组系数的优化以及对肽长度和疏水性的额外补偿产生了保留时间对疏水性的线性依赖性,R(2)值约为0.94。该模型的预测能力用于区分m / z值接近的肽段,并用于选定蛋白质的详细肽段定位。它的适用性已在从纳米孔径到窄孔径的不同尺寸的色谱柱上进行了测试,可用于直接进样或通过预柱进样。它可用于准确预测胰蛋白酶肽在具有线性水-ACN梯度和TFA作为离子对修饰剂的不同尺寸的反相(300-A孔径)色谱柱上的保留时间。

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