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Accurate Assessment of Amino Acid Mass Isotopomer Distributions for Metabolic Flux Analysis

机译:代谢通量分析的氨基酸质量同位素异构体分布的准确评估

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Metabolic flux analysis based on stable-isotope labeling experiments and analysis of mass isotopomer distributions (MID) of cellular metabolites is a tool of great significance for metabolic engineering and study of human disease.This method relies on accurate and precise measurements of mass isotopomers by gas chromatogra-phy/mass spectrometry.To improve flux estimates,we assessed potential errors in determining MID of tert-butyldimethylsilyl-derivatized amino acids,which were attributed to (i) the choice of integration algorithm,(ii) concentration effects,and (iii) overlapping fragments.We report 29 amino acid fragments that are useful for flux analysis and another 18 fragments that should be rejected,most importantly Val-302,Leu-200,Leu-302,Ile-302,Ser-302,and Asp-316.In addition,we provide a protocol to minimize errors for determining MID to less than 0.4 mol % for accepted fragments.
机译:基于稳定同位素标记实验的代谢通量分析和细胞代谢产物质量同位素异构体分布(MID)的分析,对人体的代谢工程和研究具有重要意义,该方法依赖于通过气体准确,精确地测量质量同位素异构体。为了提高通量估计值,我们评估了确定叔丁基二甲基甲硅烷基衍生氨基酸的MID的潜在误差,这归因于(i)积分算法的选择,(ii)浓度效应和(iii) )重叠的片段。我们报告了29个氨基酸片段,可用于通量分析,另外18个片段应被拒绝,最重要的是Val-302,Leu-200,Leu-302,Ile-302,Ser-302和Asp- 316.另外,我们提供了一种协议,可将用于确定可接受的片段的MID的误差降至最低0.4摩尔%。

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