Multimodal joint deconvolution and integrative signature selection in proteomics

Author:

Pan Yue,Wang XushengORCID,Sun Jiao,Liu ChunyuORCID,Peng JunminORCID,Li QianORCID

Abstract

AbstractDeconvolution is an efficient approach for detecting cell-type-specific (cs) transcriptomic signals without cellular segmentation. However, this type of methods may require a reference profile from the same molecular source and tissue type. Here, we present a method to dissect bulk proteome by leveraging tissue-matched transcriptome and proteome without using a proteomics reference panel. Our method also selects the proteins contributing to the cellular heterogeneity shared between bulk transcriptome and proteome. The deconvoluted result enables downstream analyses such as cs-protein Quantitative Trait Loci (cspQTL) mapping. We benchmarked the performance of this multimodal deconvolution approach through CITE-seq pseudo bulk data, a simulation study, and the bulk multi-omics data from human brain normal tissues and breast cancer tumors, individually, showing robust and accurate cell abundance quantification across different datasets. This algorithm is implemented in a tool MICSQTL that also provides cspQTL and multi-omics integrative visualization, available at https://bioconductor.org/packages/MICSQTL.

Funder

U.S. Department of Health & Human Services | NIH | National Cancer Institute

American Lebanese Syrian Associated Charities

Foundation for the National Institutes of Health

Publisher

Springer Science and Business Media LLC

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