MethNet: a robust approach to identify regulatory hubs and their distal targets in cancer

Author:

Skok Jane1ORCID,Sakellaropoulos Theodore1,Do Catherine2,Jiang Guimei2,Cova GiuliaORCID,Meyn Peter2,Dimartino Dacia2,Ramaswami Sitharam3,Heguy Adriana4ORCID,Tsirigos Aristotelis5ORCID

Affiliation:

1. New York University Langone Medical Center

2. NYU School of Medicine

3. NYU Langone Health

4. New York University Langone Health

5. NYU Grossman School of Medicine

Abstract

Abstract Aberrations in the capacity of DNA/chromatin modifiers and transcription factors to bind non-coding regions can lead to changes in gene regulation and impact disease phenotypes. However, identifying distal regulatory elements and connecting them with their target genes remains challenging. Here, we present MethNet, a pipeline that integrates large-scale DNA methylation and gene expression data across multiple cancers, to uncover novel cis regulatory elements (CREs) in a 1Mb region around every promoter in the genome. MethNet identifies clusters of highly ranked CREs, referred to as ‘hubs’, which contribute to the regulation of multiple genes and significantly affect patient survival. Promoter-capture Hi-C confirmed that highly ranked associations involve physical interactions between CREs and their gene targets, and CRISPRi based scRNA Perturb-seq validated the functional impact of CREs. Thus, MethNet-identified CREs represent a valuable resource for unraveling complex mechanisms underlying gene expression, and for prioritizing the verification of predicted non-coding disease hotspots.

Publisher

Research Square Platform LLC

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