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利用微粒体代谢产物生成策略,通过液相色谱-质谱联用技术促进内源性代谢物的鉴定。

Strategy of using microsome-based metabolite production to facilitate the identification of endogenous metabolites by liquid chromatography mass spectrometry.

机构信息

Department of Chemistry, University of Alberta, Edmonton, Alberta, Canada.

出版信息

Anal Chim Acta. 2011 Jan 24;685(1):36-44. doi: 10.1016/j.aca.2010.11.014. Epub 2010 Nov 24.

DOI:10.1016/j.aca.2010.11.014
PMID:21168549
Abstract

One of the challenges in metabolomic profiling of complex biological samples is to identify new and unknown compounds. Typically, standards are used to help identify metabolites, yet standards cannot be purchased or readily synthesized for many unknowns. In this work we present a strategy of using human liver microsomes (HLM) to metabolize known endogenous human metabolites (substrates), producing potentially new metabolites that have yet to be documented. The metabolites produced by HLM can be tentatively identified based on the associated substrate structure, known metabolic processes, tandem mass spectrometry (MS/MS) fragmentation patterns and, if necessary, accurate mass measurements. Once identified, these metabolites can be used as references for identification of the same compounds in complex biological samples. As a proof of principle, a total of 9 metabolites have been identified from individual HLM incubations using 5 different substrates. Each metabolite was used as a standard. In the analysis of human urine sample by liquid chromatography MS/MS, four spectral matches were found from the 9 microsome-produced metabolite standards. Two of them have previously been documented as endogenous human metabolites, the third is an isomer of a microsome-metabolite and the fourth compound has not been previously reported and is also an isomer of a microsome-metabolite. This work illustrates the feasibility of using microsome-based metabolism to produce metabolites of endogenous human metabolites that can be used to facilitate the identification of unknowns in biological samples. Future work on improving the performance of this strategy is also discussed.

摘要

在复杂生物样本的代谢组学分析中,一个挑战是鉴定新的和未知的化合物。通常,使用标准品来帮助鉴定代谢物,但对于许多未知物,标准品无法购买或容易合成。在这项工作中,我们提出了一种使用人肝微粒体(HLM)代谢已知内源性人代谢物(底物)的策略,产生尚未记录的潜在新代谢物。基于相关底物结构、已知代谢途径、串联质谱(MS/MS)碎片模式,以及在必要时进行精确质量测量,可以对 HLM 产生的代谢物进行初步鉴定。一旦鉴定出来,这些代谢物就可以用作鉴定复杂生物样本中相同化合物的参考。作为原理验证,使用 5 种不同的底物在单个 HLM 孵育中鉴定出了 9 种代谢物。每种代谢物都被用作标准品。在对人尿液样本进行液相色谱 MS/MS 分析时,从 9 种微粒体产生的代谢物标准品中发现了 4 个光谱匹配。其中两种以前被记录为内源性人代谢物,第三种是微粒体代谢物的异构体,第四种化合物以前没有报道过,也是微粒体代谢物的异构体。这项工作说明了使用基于微粒体的代谢来产生内源性人代谢物的代谢物的可行性,这可以促进生物样本中未知物的鉴定。还讨论了改进该策略性能的未来工作。

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