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Melanoma cells replicate through chemotherapy by reducing levels of key homologous recombination protein RAD51 and increasing expression of translesion synthesis DNA polymerase ζ

机译:黑色素瘤细胞通过降低关键同源重组蛋白RAD51的水平并增加跨病变合成DNA聚合酶ζ的表达通过化疗复制

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摘要

BackgroundThe global incidence of melanoma has been increasing faster than any other form of cancer. New therapies offer exciting prospects for improved survival, but the development of resistance is a major problem and there remains a need for additional effective melanoma therapy. Platinum compounds, such as cisplatin, are the most effective chemotherapeutics for a number of major cancers, but are ineffective on metastatic melanoma. They cause monofunctional adducts and intrastrand crosslinks that are repaired by nucleotide excision repair, as well as the more toxic interstrand crosslinks that are repaired by a combination of nuclease activity and homologous recombination.
机译:背景技术全球黑色素瘤的发病率增长速度超过任何其他形式的癌症。新疗法为改善生存率提供了令人兴奋的前景,但是耐药性的发展是一个主要问题,因此仍然需要其他有效的黑色素瘤疗法。铂化合物(例如顺铂)是许多主要癌症中最有效的化学疗法,但对转移性黑色素瘤无效。它们会导致单功能加合物和链内交联键(通过核苷酸切除修复修复),以及毒性更强的链间交联键(通过核酸酶活性和同源重组的组合修复)。

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