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Batch effect exerts a bigger influence on the rat urinary metabolome and gut microbiota than uraemia: a cautionary tale

机译:批量效应对大鼠尿代谢和肠道微生物群产生更大的影响,而不是铀症:一个警示的故事

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Rodent models are invaluable for studying biological processes in the context of whole organisms. The reproducibility of such research is based on an assumption of metabolic similarity between experimental animals, controlled for by breeding and housing strategies that minimise genetic and environmental variation. Here, we set out to demonstrate the effect of experimental uraemia on the rat urinary metabolome and gut microbiome but found instead that the effect of vendor shipment batch was larger in both areas than that of uraemia. Twenty four Wistar rats obtained from the same commercial supplier in two separate shipment batches underwent either subtotal nephrectomy or sham procedures. All animals undergoing subtotal nephrectomy developed an expected uraemic phenotype. The urinary metabolome was studied using 1H-NMR spectroscopy and found to vary significantly between animals from different batches, with substantial differences in concentrations of a broad range of substances including lactate, acetate, glucose, amino acids, amines and benzoate derivatives. In animals from one batch, there was a complete absence of the microbiome-associated urinary metabolite hippurate, which was present in significant concentrations in animals from the other batch. These differences were so prominent that we would have drawn quite different conclusions about the effect of uraemia on urinary phenotype depending on which batch of animals we had used. Corresponding differences were seen in the gut microbiota between animals in different batches when assessed by the sequencing of 16S rRNA gene amplicons, with higher alpha diversity and different distributions of Proteobacteria subtaxa and short-chain fatty acid producing bacteria in the second batch compared to the first. Whilst we also demonstrated differences in both the urinary metabolome and gut microbiota associated with uraemia, these effects were smaller in size than those associated with shipment batch. These results challenge the assumption that experimental animals obtained from the same supplier are metabolically comparable, and provide metabolomic evidence that batch-to-batch variations in the microbiome of experimental animals are significant confounders in an experimental study. We discuss strategies for reducing such variability and the need for transparency in research publications about the supply of experimental animals.
机译:啮齿动物模型对于在整个生物体的背景下研究生物过程非常宝贵。这种研究的再现性是基于实验动物之间代谢相似性的假设,通过育种和环境变异最小化的育种和住房策略来控制。在这里,我们开始证明实验性尿动瘤对大鼠尿代谢和肠道微生物组的影响,但发现,在两个区域的供应商出货批次的效果比尿血症的影响更大。从两种单独的装运批次中从同一商业供应商获得二十四只WISTAR大鼠,经历了小肾切除术或假手术。所有脑梗塞肾切除术的动物都开发了预期的血症表型。使用1H-NMR光谱研究尿代谢物,发现来自不同批次的动物之间的显着变化,具有较大范围物质的浓度差异,包括乳酸乳酸,乙酸盐,葡萄糖,氨基酸,胺和苯甲酸苯衍生物。在一种批次中的动物中,完全没有微生物组相关的尿代谢物海藻,其存在于来自其他批次的动物中的显着浓度。这些差异如此突出,我们将根据我们使用的批次批次的动物征收尿血症对泌尿表型的影响。当通过16S rRNA基因扩增子的测序评估时,在不同批次的动物之间的肠道微生物群中看到了相应的差异,与第一个分批的α多样性和不同的植物亚塔克萨和短链脂肪酸产生细菌的不同分布。虽然我们还证明了尿代谢和肠道微生物群的差异,但这些效果的尺寸小于与装运批次相关的影响。这些结果挑战了从同一供应商获得的实验动物是代谢可比的假设,并提供代谢组证据,即实验动物微生物组的分批变化在实验研究中是显着的混血。我们讨论降低这些可变性和对实验动物供应的研究出版物透明度的策略。

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