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Bayesian outcome-guided multi-view mixture models with applications in molecular precision medicine

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arxiv 2303.00318 v1 pith:YXEQPYDW submitted 2023-03-01 stat.ME stat.APstat.ML

Bayesian outcome-guided multi-view mixture models with applications in molecular precision medicine

classification stat.ME stat.APstat.ML
keywords clusteringdifferentbayesiandatasetsdistinctmedicinemixtureprocesses
verification ladder T0 review T1 audit T2 compute T3 formal T4 reserved
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Clustering is commonly performed as an initial analysis step for uncovering structure in 'omics datasets, e.g. to discover molecular subtypes of disease. The high-throughput, high-dimensional nature of these datasets means that they provide information on a diverse array of different biomolecular processes and pathways. Different groups of variables (e.g. genes or proteins) will be implicated in different biomolecular processes, and hence undertaking analyses that are limited to identifying just a single clustering partition of the whole dataset is therefore liable to conflate the multiple clustering structures that may arise from these distinct processes. To address this, we propose a multi-view Bayesian mixture model that identifies groups of variables (``views"), each of which defines a distinct clustering structure. We consider applications in stratified medicine, for which our principal goal is to identify clusters of patients that define distinct, clinically actionable disease subtypes. We adopt the semi-supervised, outcome-guided mixture modelling approach of Bayesian profile regression that makes use of a response variable in order to guide inference toward the clusterings that are most relevant in a stratified medicine context. We present the model, together with illustrative simulation examples, and examples from pan-cancer proteomics. We demonstrate how the approach can be used to perform integrative clustering, and consider an example in which different 'omics datasets are integrated in the context of breast cancer subtyping.

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