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Metagenomic systems biology and metabolic modeling of the human microbiome

机译:人类微生物组的元基因组系统生物学和代谢建模

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摘要

The human microbiome is a key contributor to health and development. Yet little is known about the ecological forces that are at play in defining the composition of such host-associated communities. Metagenomics-based studies have uncovered clear patterns of community structure but are often incapable of distinguishing alternative structuring paradigms. In a recent study, we integrated metagenomic analysis with a systems biology approach, using a reverse ecology framework to model numerous human microbiota species and to infer metabolic interactions between species. Comparing predicted interactions with species composition data revealed that the assembly of the human microbiome is dominated at the community level by habitat filtering. Furthermore, we demonstrated that this habitat filtering cannot be accounted for by known host phenotypes or by the metabolic versatility of the various species. Here we provide a summary of our findings and offer a brief perspective on related studies and on future approaches utilizing this metagenomic systems biology framework.
机译:人类微生物组是健康与发展的关键因素。对于定义这种与寄主相关的社区的构成所起的生态作用,人们知之甚少。基于元基因组学的研究发现了清晰的社区结构模式,但通常无法区分其他结构范例。在最近的研究中,我们使用系统生态学方法将宏基因组学分析与系统生物学方法相结合,使用反向生态学框架对众多人类微生物群落模型进行建模,并推断物种之间的代谢相互作用。将预测的相互作用与物种组成数据进行比较后发现,通过栖息地过滤,人类微生物组的装配在社区水平上占主导地位。此外,我们证明了这种栖息地的过滤不能由已知的宿主表型或各种物种的代谢多功能性来解释。在这里,我们总结了我们的发现,并简要介绍了相关研究以及利用这种宏基因组学系统生物学框架的未来方法。

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