利用低氧样抑制对同源定向DNA修复的影响。

IF 12.1 1区 医学 Q1 ONCOLOGY
Gary Altwerger , Maddie Ghazarian , Peter M. Glazer
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引用次数: 0

摘要

缺氧是肿瘤微环境的一个显著特征,可促进突变和不稳定性。这种突变负担的增加是DNA修复系统下调的结果。DNA损伤反应的缺陷可以用来诱导细胞毒性和治疗晚期癌症。随着精准医学的出现,诸如聚(adp -核糖)聚合酶(PARP)抑制剂等药物已被用于在同源定向修复(HDR)缺陷癌症中实现合成致死性。然而,大多数癌症缺乏这些预测性生物标志物。对HDR熟练人群的治疗是一个重要的未满足的临床需求。在精通HDR的背景下,人们一直对使用抗血管生成药物促进肿瘤缺氧和诱导缺乏感兴趣。例如,使用cediranib来抑制PDGFR和下调HDR通路的酶,可以与PARP抑制剂协同使用。这种组合可以改善HDR熟练癌症的治疗反应。临床前结果和II期和III期临床试验数据支持这些药物联合使用疗效的机制基础。未来的研究应该探索cediranib和其他抗血管生成药物与PARP抑制剂的有效性,以引发抗肿瘤反应并使癌症对免疫治疗敏感。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Harnessing the effects of hypoxia-like inhibition on homology-directed DNA repair

Hypoxia is a hallmark feature of the tumor microenvironment which can promote mutagenesis and instability. This increase in mutational burden occurs as a result of the downregulation of DNA repair systems. Deficits in the DNA damage response can be exploited to induce cytotoxicity and treat advanced stage cancers. With the advent of precision medicine, agents such as Poly (ADP-ribose) polymerase (PARP) inhibitors have been used to achieve synthetic lethality in homology directed repair (HDR) deficient cancers. However, most cancers lack these predictive biomarkers. Treatment for the HDR proficient population represents an important unmet clinical need. There has been interest in the use of anti-angiogenic agents to promote tumor hypoxia and induce deficiency in a HDR proficient background. For example, the use of cediranib to inhibit PDGFR and downregulate enzymes of the HDR pathway can be used synergistically with a PARP inhibitor. This combination can improve therapeutic responses in HDR proficient cancers. Preclinical results and Phase II and III clinical trial data support the mechanistic rationale for the efficacy of these agents in combination. Future investigations should explore the effectiveness of cediranib and other anti-angiogenic agents with a PARP inhibitor to elicit an antitumor response and sensitize cancers to immunotherapy.

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来源期刊
Seminars in cancer biology
Seminars in cancer biology 医学-肿瘤学
CiteScore
26.80
自引率
4.10%
发文量
347
审稿时长
15.1 weeks
期刊介绍: Seminars in Cancer Biology (YSCBI) is a specialized review journal that focuses on the field of molecular oncology. Its primary objective is to keep scientists up-to-date with the latest developments in this field. The journal adopts a thematic approach, dedicating each issue to an important topic of interest to cancer biologists. These topics cover a range of research areas, including the underlying genetic and molecular causes of cellular transformation and cancer, as well as the molecular basis of potential therapies. To ensure the highest quality and expertise, every issue is supervised by a guest editor or editors who are internationally recognized experts in the respective field. Each issue features approximately eight to twelve authoritative invited reviews that cover various aspects of the chosen subject area. The ultimate goal of each issue of YSCBI is to offer a cohesive, easily comprehensible, and engaging overview of the selected topic. The journal strives to provide scientists with a coordinated and lively examination of the latest developments in the field of molecular oncology.
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