Rational combination therapy for hepatocellular carcinoma with PARP1 and DNA-PK inhibitors.
Chen WangHuanyin TangAnke GengBinghua DaiHaiping ZhangXiaoxiang SunYu ChenZhibing QiaoHong ZhuJiamei YangJiayu ChenQizhi HeNan QinJinru XieRong TanXiaoping WanShao-Rong GaoYing JiangFang-Lin SunZhiyong MaoPublished in: Proceedings of the National Academy of Sciences of the United States of America (2020)
Understanding differences in DNA double-strand break (DSB) repair between tumor and normal tissues would provide a rationale for developing DNA repair-targeted cancer therapy. Here, using knock-in mouse models for measuring the efficiency of two DSB repair pathways, homologous recombination (HR) and nonhomologous end-joining (NHEJ), we demonstrated that both pathways are up-regulated in hepatocellular carcinoma (HCC) compared with adjacent normal tissues due to altered expression of DNA repair factors, including PARP1 and DNA-PKcs. Surprisingly, inhibiting PARP1 with olaparib abrogated HR repair in HCC. Mechanistically, inhibiting PARP1 suppressed the clearance of nucleosomes at DNA damage sites by blocking the recruitment of ALC1 to DSB sites, thereby inhibiting RPA2 and RAD51 recruitment. Importantly, combining olaparib with NU7441, a DNA-PKcs inhibitor that blocks NHEJ in HCC, synergistically suppressed HCC growth in both mice and HCC patient-derived-xenograft models. Our results suggest the combined inhibition of both HR and NHEJ as a potential therapy for HCC.
Keyphrases
- dna repair
- dna damage
- cancer therapy
- combination therapy
- dna damage response
- circulating tumor
- signaling pathway
- cell free
- single molecule
- gene expression
- oxidative stress
- mouse model
- clinical trial
- poor prognosis
- drug delivery
- nucleic acid
- transcription factor
- adipose tissue
- risk assessment
- insulin resistance
- circulating tumor cells