dCCA: detecting differential covariation patterns between two types of high-throughput omics data

Author:

Lee Hwiyoung12ORCID,Ma Tianzhou3ORCID,Ke Hongjie3,Ye Zhenyao245,Chen Shuo1245ORCID

Affiliation:

1. Maryland Psychiatric Research Center, School of Medicine, University of Maryland , Baltimore, MD 21201 , United States

2. The University of Maryland Institute for Health Computing (UM-IHC) , North Bethesda, MD 20852 , United States

3. Department of Epidemiology and Biostatistics, University of Maryland , College Park, MD 20742 , United States

4. Division of Biostatistics and Bioinformatics , Department of Epidemiology and Public Health, , Baltimore, MD 21201 , United States

5. School of Medicine, University of Maryland , Department of Epidemiology and Public Health, , Baltimore, MD 21201 , United States

Abstract

Abstract Motivation The advent of multimodal omics data has provided an unprecedented opportunity to systematically investigate underlying biological mechanisms from distinct yet complementary angles. However, the joint analysis of multi-omics data remains challenging because it requires modeling interactions between multiple sets of high-throughput variables. Furthermore, these interaction patterns may vary across different clinical groups, reflecting disease-related biological processes. Results We propose a novel approach called Differential Canonical Correlation Analysis (dCCA) to capture differential covariation patterns between two multivariate vectors across clinical groups. Unlike classical Canonical Correlation Analysis, which maximizes the correlation between two multivariate vectors, dCCA aims to maximally recover differentially expressed multivariate-to-multivariate covariation patterns between groups. We have developed computational algorithms and a toolkit to sparsely select paired subsets of variables from two sets of multivariate variables while maximizing the differential covariation. Extensive simulation analyses demonstrate the superior performance of dCCA in selecting variables of interest and recovering differential correlations. We applied dCCA to the Pan-Kidney cohort from the Cancer Genome Atlas Program database and identified differentially expressed covariations between noncoding RNAs and gene expressions. Availability and Implementation The R package that implements dCCA is available at https://github.com/hwiyoungstat/dCCA.

Funder

National Institutes of Health

Publisher

Oxford University Press (OUP)

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