Toward the human cellular microRNAome

Author:

McCall Matthew N.,Kim Min-Sik,Adil Mohammed,Patil Arun H.,Lu Yin,Mitchell Christopher J.,Leal-Rojas Pamela,Xu Jinchong,Kumar Manoj,Dawson Valina L.ORCID,Dawson Ted M.ORCID,Baras Alexander S.ORCID,Rosenberg Avi Z.ORCID,Arking Dan E.ORCID,Burns Kathleen H.,Pandey AkhileshORCID,Halushka Marc K.ORCID

Abstract

MicroRNAs are short RNAs that serve as regulators of gene expression and are essential components of normal development as well as modulators of disease. MicroRNAs generally act cell-autonomously, and thus their localization to specific cell types is needed to guide our understanding of microRNA activity. Current tissue-level data have caused considerable confusion, and comprehensive cell-level data do not yet exist. Here, we establish the landscape of human cell-specific microRNA expression. This project evaluated 8 billion small RNA-seq reads from 46 primary cell types, 42 cancer or immortalized cell lines, and 26 tissues. It identified both specific and ubiquitous patterns of expression that strongly correlate with adjacent superenhancer activity. Analysis of unaligned RNA reads uncovered 207 unknown minor strand (passenger) microRNAs of known microRNA loci and 495 novel putative microRNA loci. Although cancer cell lines generally recapitulated the expression patterns of matched primary cells, their isomiR sequence families exhibited increased disorder, suggesting DROSHA- and DICER1-dependent microRNA processing variability. Cell-specific patterns of microRNA expression were used to de-convolute variable cellular composition of colon and adipose tissue samples, highlighting one use of these cell-specific microRNA expression data. Characterization of cellular microRNA expression across a wide variety of cell types provides a new understanding of this critical regulatory RNA species.

Funder

American Heart Association

National Institutes of Health

Cancer Center Support

Laura and Isaac Perlmutter Cancer Center

NCI's Clinical Proteomic Tumor Analysis Consortium

NIH

National Fund for Scientific and Technological Development, FONDECYT

NIH/NINDS

Publisher

Cold Spring Harbor Laboratory

Subject

Genetics(clinical),Genetics

Reference59 articles.

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