Polycomb group proteins in cancer: multifaceted functions and strategies for modulation

Author:

Wang Sijie1,C. Ordonez-Rubiano Sandra1,Dhiman Alisha1,Jiao Guanming1,Strohmier Brayden P1,Krusemark Casey J1,Dykhuizen Emily C1ORCID

Affiliation:

1. Department of Medicinal Chemistry and Molecular Pharmacology, College of Pharmacy, Purdue University and Purdue University Center for Cancer Research, 201 S. University St., West Lafayette, IN 47907 USA

Abstract

Abstract Polycomb repressive complexes (PRCs) are a heterogenous collection of dozens, if not hundreds, of protein complexes composed of various combinations of subunits. PRCs are transcriptional repressors important for cell-type specificity during development, and as such, are commonly mis-regulated in cancer. PRCs are broadly characterized as PRC1 with histone ubiquitin ligase activity, or PRC2 with histone methyltransferase activity; however, the mechanism by which individual PRCs, particularly the highly diverse set of PRC1s, alter gene expression has not always been clear. Here we review the current understanding of how PRCs act, both individually and together, to establish and maintain gene repression, the biochemical contribution of individual PRC subunits, the mis-regulation of PRC function in different cancers, and the current strategies for modulating PRC activity. Increased mechanistic understanding of PRC function, as well as cancer-specific roles for individual PRC subunits, will uncover better targets and strategies for cancer therapies.

Funder

Lilly Graduate Research Award from the Purdue College of Pharmacy

NIH

ACS

Publisher

Oxford University Press (OUP)

Subject

General Medicine

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