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对曼氏血吸虫感染小鼠的毛细管电泳代谢组学实验的化学计量学和生物学验证。

Chemometric and biological validation of a capillary electrophoresis metabolomic experiment of Schistosoma mansoni infection in mice.

机构信息

Faculty of Pharmacy, San Pablo-CEU, Campus Monteprincipe, Boadilla del Monte, Madrid, Spain.

出版信息

Electrophoresis. 2010 Jul;31(14):2338-48. doi: 10.1002/elps.200900523.

Abstract

Metabonomic and metabolomic studies are increasingly utilized for biomarker identification in different fields, including biology of infection. The confluence of improved analytical platforms and the availability of powerful multivariate analysis software have rendered the multiparameter profiles generated by these omics platforms a user-friendly alternative to the established analysis methods where the quality and practice of a procedure is well defined. However, unlike traditional assays, validation methods for these new multivariate profiling tools have yet to be established. We propose a validation for models obtained by CE fingerprinting of urine from mice infected with the blood fluke Schistosoma mansoni. We have analysed urine samples from two sets of mice infected in an inter-laboratory experiment where different infection methods and animal husbandry procedures were employed in order to establish the core biological response to a S. mansoni infection. CE data were analysed using principal component analysis. Validation of the scores consisted of permutation scrambling (100 repetitions) and a manual validation method, using a third of the samples (not included in the model) as a test or prediction set. The validation yielded 100% specificity and 100% sensitivity, demonstrating the robustness of these models with respect to deciphering metabolic perturbations in the mouse due to a S. mansoni infection. A total of 20 metabolites across the two experiments were identified that significantly discriminated between S. mansoni-infected and noninfected control samples. Only one of these metabolites, allantoin, was identified as manifesting different behaviour in the two experiments. This study shows the reproducibility of CE-based metabolic profiling methods for disease characterization and screening and highlights the importance of much needed validation strategies in the emerging field of metabolomics.

摘要

代谢组学和代谢组学研究越来越多地用于不同领域的生物标志物识别,包括感染生物学。改进的分析平台和强大的多元分析软件的可用性,使得这些组学平台生成的多参数谱成为替代传统分析方法的用户友好选择,传统分析方法中,程序的质量和实践已经得到了很好的定义。然而,与传统的分析方法不同,这些新的多元分析工具的验证方法尚未建立。我们提出了一种用于验证从感染曼氏血吸虫的小鼠尿液中进行 CE 指纹图谱分析获得的模型的方法。我们分析了两组在实验室间实验中感染的小鼠的尿液样本,其中采用了不同的感染方法和动物饲养程序,以确定对曼氏血吸虫感染的核心生物学反应。CE 数据采用主成分分析进行分析。评分的验证包括置换混淆(重复 100 次)和手动验证方法,使用三分之一的样本(不包括在模型中)作为测试或预测集。验证结果为 100%特异性和 100%灵敏度,证明了这些模型在破译由于曼氏血吸虫感染而导致的小鼠代谢紊乱方面的稳健性。在两个实验中总共鉴定出 20 种代谢物,它们可以显著区分曼氏血吸虫感染和非感染对照样本。这 20 种代谢物中只有一种,即尿囊素,在两个实验中表现出不同的行为。这项研究表明了基于 CE 的代谢谱分析方法用于疾病特征描述和筛选的可重复性,并强调了在新兴的代谢组学领域中需要验证策略的重要性。

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