A large-scale cancer-specific protein–DNA interaction network

Author:

Lu Yunwei1ORCID,Berenson Anna12,Lane Ryan1ORCID,Guelin Isabelle1ORCID,Li Zhaorong3,Chen Yilin1,Shah Sakshi1,Yin Meimei1,Soto-Ugaldi Luis Fernando4ORCID,Fiszbein Ana123,Fuxman Bass Juan Ignacio123ORCID

Affiliation:

1. Biology Department, Boston University

2. Molecular Biology, Cellular Biology and Biochemistry Program, Boston University

3. Bioinformatics Program, Boston University

4. Tri-Institutional Program in Computational Biology and Medicine, New York, NY, USA

Abstract

Cancer development and progression are generally associated with gene dysregulation, often resulting from changes in the transcription factor (TF) sequence or expression. Identifying key TFs involved in cancer gene regulation provides a framework for potential new therapeutics. This study presents a large-scale cancer gene TF-DNA interaction network, as well as an extensive promoter clone resource for future studies. Highly connected TFs bind to promoters of genes associated with either good or poor cancer prognosis, suggesting that strategies aimed at shifting gene expression balance between these two prognostic groups may be inherently complex. However, we identified potential for oncogene-targeted therapeutics, with half of the tested oncogenes being potentially repressed by influencing specific activators or bifunctional TFs. Finally, we investigate the role of intrinsically disordered regions within the key cancer-related TF ESR1 in DNA binding and transcriptional activity, and found that these regions can have complex trade-offs in TF function. Altogether, our study broadens our knowledge of the TFs involved in cancer gene regulation and provides a valuable resource for future studies and therapeutics.

Funder

National Institute of General Medical Sciences

HHS | NIH | National Cancer Institute

HHS | NIH | National Institute of General Medical Sciences

Publisher

Life Science Alliance, LLC

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