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    Temporal and Causal Inference with Longitudinal Multi-omics Microbiome Data

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    Microbiomes are communities of microbes inhabiting an environmental niche. Thanks to next generation sequencing technologies, it is now possible to study microbial communities, their impact on the host environment, and their role in specific diseases and health. Technology has also triggered the increased generation of multi-omics microbiome data, including metatranscriptomics (quantitative survey of the complete metatranscriptome of the microbial community), metabolomics (quantitative profile of the entire set of metabolites present in the microbiome\u27s environmental niche), and host transcriptomics (gene expression profile of the host). Consequently, another major challenge in microbiome data analysis is the integration of multi-omics data sets and the construction of unified models. Finally, since microbiomes are inherently dynamic, to fully understand the complex interactions that take place within these communities, longitudinal studies are critical. Although the analysis of longitudinal microbiome data has been attempted, these approaches do not attempt to probe interactions between taxa, do not offer holistic analyses, and do not investigate causal relationships. In this work we propose approaches to address all of the above challenges. We propose novel analysis pipelines to analyze multi-omic longitudinal microbiome data, and to infer temporal and causal relationships between the different entities involved. As a first step, we showed how to deal with longitudinal metagenomic data sets by building a pipeline, PRIMAL, which takes microbial abundance data as input and outputs a dynamic Bayesian network model that is highly predictive, suggests significant interactions between the different microbes, and proposes important connections from clinical variables. A significant innovation of our work is its ability to deal with differential rates of the internal biological processes in different individuals. Second, we showed how to analyze longitudinal multi-omic microbiome datasets. Our pipeline, PALM, significantly extends the previous state of the art by allowing for the integration of longitudinal metatranscriptomics, host transcriptomics, and metabolomics data in additional to longitudinal metagenomics data. PALM achieves prediction powers comparable to the PRIMAL pipeline while discovering a web of interactions between the entities of far greater complexity. An important innovation of PALM is the use of a multi-omic Skeleton framework that incorporates prior knowledge in the learning of the models. Another major innovation of this work is devising a suite of validation methods, both in silico and in vitro, enhancing the utility and validity of PALM. Finally, we propose a suite of novel methods (unrolling and de-confounding), called METALICA, consisting of tools and techniques that make it possible to uncover significant details about the nature of microbial interactions. We also show methods to validate such interactions using ground truth databases. The proposed methods were tested using an IBD multi-omics dataset
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