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Strategies to prevent anthracycline-induced cardiotoxicity in cancer survivors

机译:预防蒽环素诱导的癌症幸存者心脏毒性的策略

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Cancer diagnostics and therapies have improved steadily over the last few decades, markedly increasing life expectancy for patients at all ages. However, conventional and newer anti-neoplastic therapies can cause short- and long-term cardiotoxicity. The clinical implications of this cardiotoxicity become more important with the increasing use of cardiotoxic drugs. The implications are especially serious among patients predisposed to adverse cardiac effects, such as youth, the elderly, those with cardiovascular comorbidities, and those receiving additional chemotherapies or thoracic radiation. However, the optimal strategy for preventing and managing chemotherapy-induced cardiotoxicity remains unknown. The routine use of neurohormonal antagonists for cardioprotection is not currently justified, given the marginal benefits and associated adverse events, particularly with long-term use. The only United States Food and Drug Administration and European Medicines Agency approved treatment for preventing anthracycline-related cardiomyopathy is dexrazoxane. We advocate administering dexrazoxane during cancer treatment to limit the cardiotoxic effects of anthracycline chemotherapy.
机译:在过去的几十年中,癌症诊断和疗法稳步地改善,显着增加了所有年龄段的患者的预期寿命。然而,常规和较新的抗肿瘤疗法可能导致短期和长期心脏毒性。这种心脏毒性的临床意义随着心脏毒性药物的增加而变得更加重要。倾向于不良心脏效应的患者,如青年,老年人,心血管合并症那些人,以及接受额外的化疗或胸部辐射的患者尤其严重。然而,用于预防和管理化疗诱导的心脏毒性的最佳策略仍然未知。鉴于边际益处和相关不良事件,鉴于边际益处和相关不良事件,目前常规使用神经外异常拮抗剂的常规使用。唯一的美国食品和药物管理局和欧洲药物局批准用于预防蒽环类相关的心肌病的治疗是甲氧烷。我们提倡在癌症治疗过程中施用甲氧烷,以限制蒽环类化疗的心脏毒性作用。

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