BRD4 inhibition impairs DNA mismatch repair, induces mismatch repair mutation signatures and creates therapeutic vulnerability to immune checkpoint blockade in MMR-proficient tumors.
Yu FuBin YangYaoyuan CuiXingyuan HuXi LiFunian LuTianyu QinLi ZhangZhe HuEnsong GuoJunpeng FanRourou XiaoWenting LiXu QinDianxing HuWenju PengJingbo LiuBeibei WangGordon B MillsGang ChenChaoyang SunPublished in: Journal for immunotherapy of cancer (2023)
We demonstrated that BRD4 inhibition suppressed expression of genes critical to MMR, dampened MMR, and increased dMMR mutation signatures both in vitro and in vivo, sensitizing pMMR tumors to ICB. Importantly, even in BRD4 inhibitors (BRD4i)-resistant tumor models, the effects of BRD4i on MMR function were maintained rendering tumors sensitive to ICB. Together, these data identified a strategy to induce dMMR in pMMR tumors and further, indicated that BRD4i sensitive and resistant tumors could benefit from immunotherapy.