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Targeting bromodomain protein ANCCA/ATAD2 enhances the efficacy of DNA-damaging chemotherapy agents and radiation

机译:靶向溴琼蛋白ANCCA / ATAD2增强DNA损伤化疗药物和辐射的功效

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摘要

Bromodomain proteins such as BRD4 chromatin regulator are attractive cancer therapeutic targets. ANCCA (AAA+ nuclear coregulatory cancer-associated protein, also known as ATPase family AAA domain containing 2 or ATAD2) is a novel oncology drug target and contains a bromodomain and an ATPase domain. Our research group as well as others previously identified ANCCA/ATAD2 as a putative oncogene and a poor prognosis factor in many types of cancer including triple-negative breast cancer (TNBC). In the present study, it is reported for the first time that the expression of ANCCA was highly induced by DNA-damaging chemotherapy agents such as carboplatin, doxorubicin and mitomycin C, as well as ionizing radiation. Notably, ANCCA is required for efficient dissolution of DNA damage foci and homologous recombination. Further studies revealed that ANCCA mediates the optimal expression and activation of DNA damage response and repair factors including Chk1, Chk2 and BRCA1, and that ANCCA is recruited to the promoter of BRCA1 in response to DNA damage. Moreover, ANCCA knockdown sensitizes TNBC cells to carboplatin. Collectively, these data provide the first evidence indicating that ANCCA is a novel mediator of DNA damage response and repair and that targeting ANCCA can enhance the efficacy of radiation and chemotherapies.
机译:BRD4染色质调节剂如BROMODOMAIN蛋白是有吸引力的癌症治疗靶标。 ANCCA(AAA +核心核癌症相关蛋白,也称为ATP酶系列AAA结构域的含有2或ATAD2)是一种新型肿瘤药物靶标,含有溴琼酶和ATPase结构域。我们的研究组以及以前认为ANCCA / ATAD2的其他癌症和许多类型癌症中的预测因素差,包括三阴性乳腺癌(TNBC)。在本研究中,首次报道了ANCCA的表达高度诱导的DNA损伤化疗剂如卡铂,多柔比霉素和丝霉素C,以及电离辐射。值得注意的是,ANCCA是有效溶解DNA损伤焦点和同源重组的有效溶解。进一步的研究表明,ANCCA介导DNA损伤反应和修复因子的最佳表达和激活,包括CHK1,CHK2和BRCA1,并且响应DNA损伤征集ANCA1的启动子。此外,ANCCA敲低敏化TNBC细胞到卡铂。总的来说,这些数据提供了第一种证据,表明ANCCA是DNA损伤反应和修复的新型介质,靶向ANCCA可以增强辐射和化疗的疗效。

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