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<i>PARP1</i> and <i>PRC2</i> double deficiency promotes <i>BRCA</i>‐proficient breast cancer growth by modification of the tumor microenvironment

A‐Yeong Yang, Eun‐Bee Choi, Mi So Park, Seon‐Kyu Kim, Minseok Park, Mi‐Young Kim

2020FEBS Journal17 citationsDOIOpen Access PDF

Abstract

Poly (ADP-ribose) polymerase 1 (PARP1) and polycomb-repressive complex 2 (PRC2) are each known for their individual roles in cancer, but their cooperative roles have only been studied in the DNA damage repair process in the context of BRCA-mutant cancers. Here, we show that simultaneous inhibition of PARP1 and PRC2 in the MDA-MB-231 BRCA-proficient triple-negative breast cancer (TNBC) cell line leads to a synthetic viability independent of the mechanisms of DNA damage repair. Specifically, we find that either genetic depletion or pharmacological inhibition of both PARP1 and PRC2 can accelerate tumor growth rate. We attribute this to modifications in the tumor microenvironment (TME) that are induced by double-depleted breast cancer cells, such as promoting intratumoral angiogenesis and increasing the proportion of tumor-promoting type 2 (M2) macrophages. These changes subsequently inhibit cell death and promote proliferation. Mechanistically, we find that PARP1 and PRC2 double depletion induces not only a basal activation of the NF-κB pathway but also a maximal activation of NF-κB within the TME in response to external stimuli such as hypoxia and the presence of macrophages. In summary, our study reveals an unprecedented synthetic viable interaction between PARP1 and PRC2 in BRCA-proficient TNBC and identifies NF-κB as the downstream mediator. DATABASE: RNA-seq data are available in the GEO databases under the accession GSE142769.

Topics & Concepts

PARP1Cancer researchTumor microenvironmentTriple-negative breast cancerPRC2AngiogenesisPoly ADP ribose polymeraseCancerDNA damageBiologyBreast cancerChemistryEZH2PolymeraseDNAChromatinGeneticsTumor cellsPARP inhibition in cancer therapyDNA Repair MechanismsRNA Research and Splicing