聚(ADP-核糖)聚合酶抑制剂 AG014699 在突变或甲基化 BRCA1 或 BRCA2 的人类癌症中的治疗潜力。
Therapeutic potential of poly(ADP-ribose) polymerase inhibitor AG014699 in human cancers with mutated or methylated BRCA1 or BRCA2.
机构信息
Northern Institute for Cancer Research, University of Newcastle Upon Tyne, Medical School, Newcastle Upon Tyne, NE2 4HH, UK.
出版信息
J Natl Cancer Inst. 2011 Feb 16;103(4):334-46. doi: 10.1093/jnci/djq509. Epub 2010 Dec 23.
BACKGROUND
Mutations in BRCA1 and BRCA2 (BRCA1/2), components of the homologous recombination DNA repair (HRR) pathway, are associated with hereditary breast and ovarian cancers. Poly(ADP-ribose) polymerase (PARP) inhibitors are selectively cytotoxic to animal cells with defective HRR, but results in human cancer cells have been contradictory. We undertook, to our knowledge, the first comprehensive in vitro and in vivo investigations of the antitumor activity of the PARP inhibitor AG014699 in human cancer cells carrying mutated or epigenetically silenced BRCA1/2.
METHODS
We used nine human cell lines, four with nonmutated BRCA1/2 (MCF7, MDA-MB-231, and HCC1937-BRCA1 [breast cancer] and OSEC-2 [ovarian surface epithelial]), two with mutated BRCA1 (MDA-MB-436 and HCC1937 [breast cancer]), one with mutated BRCA2 (CAPAN-1 [pancreatic cancer]), one that was heterozygous for BRCA2 (OSEC-1 [ovarian surface epithelial]), and one with epigenetically silenced BRCA1 (UACC3199 [breast cancer]), and two Chinese hamster ovary cell lines, parental AA8 and XRCC3 mutated IRS 1SF. We assessed cytotoxicity, DNA damage, and HRR function. Antitumor activity of AG014699 was determined by growth of xenograft tumors (five mice per treatment group). Long-term safety of AG014699 was assessed.
RESULTS
AG014699 (≤10 μM) was cytotoxic to cells with mutated BRCA1/2 or XRCC3 and to UACC3199 cells with epigenetically silenced BRCA1 but not to cells without BRCA1/2 or XRCC3 mutations or that were heterozygous for BRCA2 mutation. AG014699 induced DNA double-strand breaks in all nine cell lines studied. HRR was observed only in cells with functional BRCA1/2 proteins. Growth of xenograft tumors with BRCA1/2 mutations or with epigenetically silenced BRCA1 was reduced by AG014699 treatment, and combination treatment with AG014699 plus carboplatin was more effective than either drug alone. AG014699 was not toxic in mice with nonmutated or heterozygous BRCA2.
CONCLUSION
Human cancer cells or xenograft tumors with mutated or epigenetically silenced BRCA1/2 were sensitive to AG014699 monotherapy, indicating a potential role for PARP inhibitors in sporadic human cancers.
背景
BRCA1 和 BRCA2(BRCA1/2)基因的突变与遗传性乳腺癌和卵巢癌有关,它们是同源重组 DNA 修复(HRR)途径的组成部分。聚(ADP-核糖)聚合酶(PARP)抑制剂对 HRR 功能缺陷的动物细胞具有选择性细胞毒性,但在人类癌细胞中的结果却相互矛盾。我们首次进行了全面的体外和体内研究,以评估 PARP 抑制剂 AG014699 在携带突变或表观遗传沉默 BRCA1/2 的人类癌细胞中的抗肿瘤活性。
方法
我们使用了 9 个人类细胞系,其中 4 个细胞系的 BRCA1/2 未突变(MCF7、MDA-MB-231 和 HCC1937-BRCA1[乳腺癌]和 OSEC-2[卵巢表面上皮]),2 个细胞系的 BRCA1 突变(MDA-MB-436 和 HCC1937[乳腺癌]),1 个细胞系的 BRCA2 突变(CAPAN-1[胰腺癌]),1 个细胞系的 BRCA2 杂合性缺失(OSEC-1[卵巢表面上皮]),1 个细胞系的 BRCA1 表观遗传沉默(UACC3199[乳腺癌]),以及 2 个中国仓鼠卵巢细胞系,亲本 AA8 和 XRCC3 突变 IRS 1SF。我们评估了细胞毒性、DNA 损伤和 HRR 功能。通过异种移植肿瘤的生长(每组 5 只小鼠)来确定 AG014699 的抗肿瘤活性。评估了 AG014699 的长期安全性。
结果
AG014699(≤10 μM)对携带突变 BRCA1/2 或 XRCC3 的细胞以及具有表观遗传沉默 BRCA1 的 UACC3199 细胞具有细胞毒性,但对没有 BRCA1/2 或 XRCC3 突变或 BRCA2 杂合性缺失的细胞或细胞没有细胞毒性。AG014699 诱导了所有 9 个细胞系的 DNA 双链断裂。仅在具有功能性 BRCA1/2 蛋白的细胞中观察到 HRR。携带 BRCA1/2 突变或表观遗传沉默 BRCA1 的异种移植肿瘤的生长被 AG014699 治疗所抑制,并且 AG014699 联合卡铂治疗比单独使用任何一种药物更有效。AG014699 在非突变或杂合性缺失 BRCA2 的小鼠中没有毒性。
结论
携带突变或表观遗传沉默 BRCA1/2 的人类癌细胞或异种移植肿瘤对 AG014699 单药治疗敏感,表明 PARP 抑制剂在散发性人类癌症中可能具有作用。
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