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Collateral damage: toxic effects of targeted antiangiogenic therapies in ovarian cancer.

机译:附带损害:靶向抗血管生成疗法在卵巢癌中的毒性作用。

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摘要

First-line chemotherapy fails in more than 20% of patients with epithelial ovarian cancer and about 40-50% of women who respond to initial treatment relapse within 2 years. In the recurrent setting, second-line chemotherapeutic agents have a 15-20% response rate with no cures. Fortunately, clinical investigations that have assessed the efficacy of new, biologically targeted therapies have reinvigorated therapeutic options for patients living with ovarian and other malignancies. In view of the fact that ovarian cancer is one of the most angiogenic neoplasms, there is great hope that implementing targeted agents with antiangiogenic properties will improve outcomes. However, as experience grows with the antitumour activity of these drugs, new toxic effects are emerging. The effects of antiangiogenic agents on molecules and processes that also have physiologically important roles in healthy tissues are at the crux of these toxic effects, or "collateral damage". This review discusses the leading toxic effects encountered and anticipated in clinical investigation and practice with antiangiogenic agents in patients with ovarian cancer, with particular focus on potential management strategies.
机译:一线化疗在20%以上的上皮性卵巢癌患者中无效,约40-50%的对初始治疗有反应的女性在2年内复发。在复发情况下,二线化疗药物的治愈率为15%至20%,无治愈方法。幸运的是,评估新的生物靶向疗法的疗效的临床研究为卵巢癌和其他恶性肿瘤患者提供了新的治疗选择。鉴于卵巢癌是血管生成最多的肿瘤之一,因此,寄希望于采用具有抗血管生成特性的靶向药物可以改善预后。但是,随着这些药物的抗肿瘤活性的发展,新的毒性作用正在出现。抗血管生成剂对在健康组织中也具有生理重要作用的分子和过程的作用正处于这些毒性作用或“附带损害”的症结所在。这篇综述讨论了抗血管生成剂在卵巢癌患者中在临床研究和实践中遇到和预期的主要毒性作用,特别着重于潜在的治疗策略。

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