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Quantitation of Endogenous Metabolites in Mouse Tumors Using Mass-Spectrometry Imaging

机译:用质谱成像定量小鼠肿瘤内源代谢物的定量

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摘要

Described is a quantitative-mass-spectrometry-imaging (qMSI) methodology for the analysis of lactate and glutamate distributions in order to delineate heterogeneity among mouse tumor models used to support drug-discovery efficacy testing. We evaluate and report on preanalysis-stabilization methods aimed at improving the reproducibility and efficiency of quantitative assessments of endogenous molecules in tissues. Stability experiments demonstrate that optimum stabilization protocols consist of frozen-tissue embedding, post-tissue-sectioning desiccation, and storage at ?80 °C of tissue sections sealed in vacuum-tight containers. Optimized stabilization protocols are used in combination with qMSI methodology for the absolute quantitation of lactate and glutamate in tumors, incorporating the use of two different stable-isotope-labeled versions of each analyte and spectral-clustering performed on each tissue section using k -means clustering to allow region-specific, pixel-by-pixel quantitation. Region-specific qMSI was used to screen different tumor models and identify a phenotype that has low lactate heterogeneity, which will enable accurate measurements of lactate modulation in future drug-discovery studies. We conclude that using optimized qMSI protocols, it is possible to quantify endogenous metabolites within tumors, and region-specific quantitation can provide valuable insight into tissue heterogeneity and the tumor microenvironment.
机译:描述是一种用于分析乳酸和谷氨酸分布的定量 - 质谱 - 成像(QMSI)方法,以便描绘用于支持药物发现功效测试的小鼠肿瘤模型中的异质性。我们评估并报告旨在提高组织中内源分子定量评估的再现性和效率的预序稳定方法。稳定性实验表明,最佳稳定方案由冷冻组织嵌入,组织切片干燥和储存在真空密封容器中密封的组织切片的储存。优化的稳定方案与QMSI方法组合使用,用于肿瘤中的乳酸乳酸和谷氨酸的绝对定量,掺杂使用每个分析物和光谱聚类的两种不同的稳定同位素标记的版本,使用 K在每个组织部分上进行 - 群集群集以允许特定于区域的像素逐个像素定量。地区特异性QMSI用于筛选不同的肿瘤模型,并鉴定具有低乳酸异质性的表型,这将能够准确测量未来的药物发现研究中的乳酸乳液调制。我们得出结论,使用优化的QMSI方案,可以量化肿瘤内的内源代谢物,并且区域特定的定量可以提供有价值的洞察组织异质性和肿瘤微环境。

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  • 来源
    《Analytical chemistry》 |2018年第10期|共8页
  • 作者单位

    Pathology Drug Safety &

    Metabolism IMED Biotech Unit AstraZeneca Darwin Building Cambridge Science Park Milton Road Cambridge Cambridgeshire CB4 0WG U.K.;

    National Centre of Excellence in Mass Spectrometry Imaging (NiCE-MSI) National Physical Laboratory Teddington TW11 0LW U.K.;

    Pathology Drug Safety &

    Metabolism IMED Biotech Unit AstraZeneca Darwin Building Cambridge Science Park Milton Road Cambridge Cambridgeshire CB4 0WG U.K.;

    Biomolecular Mass Spectrometry Imaging National Resource for MSI Science for Life Laboratory Department of Pharmaceutical Biosciences Uppsala University Uppsala 752 37 Sweden;

    Pathology Drug Safety &

    Metabolism IMED Biotech Unit AstraZeneca Darwin Building Cambridge Science Park Milton Road Cambridge Cambridgeshire CB4 0WG U.K.;

    Bioscience Oncology IMED Biotech Unit AstraZeneca Cambridge CB4 0WG U.K.;

    Pathology Drug Safety &

    Metabolism IMED Biotech Unit AstraZeneca Darwin Building Cambridge Science Park Milton Road Cambridge Cambridgeshire CB4 0WG U.K.;

    Bioscience Oncology IMED Biotech Unit AstraZeneca Cambridge CB4 0WG U.K.;

    Bioscience Oncology IMED Biotech Unit AstraZeneca Cambridge CB4 0WG U.K.;

    Biomolecular Mass Spectrometry Imaging National Resource for MSI Science for Life Laboratory Department of Pharmaceutical Biosciences Uppsala University Uppsala 752 37 Sweden;

    Centre for Mass Spectrometry Imaging Biomolecular Research Centre Sheffield Hallam University Sheffield S1 1WB U.K.;

    National Centre of Excellence in Mass Spectrometry Imaging (NiCE-MSI) National Physical Laboratory Teddington TW11 0LW U.K.;

    Bioscience Oncology IMED Biotech Unit AstraZeneca Cambridge CB4 0WG U.K.;

    Pathology Drug Safety &

    Metabolism IMED Biotech Unit AstraZeneca Darwin Building Cambridge Science Park Milton Road Cambridge Cambridgeshire CB4 0WG U.K.;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分析化学;
  • 关键词

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