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Oxidative stress and inflammation: determinants of anthracycline cardiotoxicity and possible therapeutic targets

机译:氧化应激和炎症:蒽环心毒性的决定因素和可能的治疗目标

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Chemotherapy with anthracycline-based regimens remains a cornerstone of treatment of many solid and blood tumors but is associated with a significant risk of cardiotoxicity, which can manifest as asymptomatic left ventricular dysfunction or overt heart failure. These effects are typically dose-dependent and cumulative and may require appropriate screening strategies and cardioprotective therapies in order to minimize changes to anticancer regimens or even their discontinuation. Our current understanding of cardiac damage by anthracyclines includes a central role of oxidative stress and inflammation. The identification of these processes through circulating biomarkers or imaging techniques might then be helpful for early diagnosis and risk stratification. Furthermore, therapeutic strategies relieving oxidative stress and inflammation hold promise to prevent heart failure development or at least to mitigate cardiac damage, although further evidence is needed on their efficacy, either alone or as part of combination therapies with neurohormonal antagonists, which are the current adopted standard.
机译:以蒽环类药物为基础的化疗方案仍然是许多实体瘤和血液肿瘤治疗的基石,但与心脏毒性的显著风险相关,其表现为无症状的左心室功能障碍或明显的心力衰竭。这些效应通常是剂量依赖性和累积性的,可能需要适当的筛查策略和心脏保护疗法,以最大限度地减少抗癌方案的改变,甚至减少其停用。我们目前对蒽环类药物心脏损害的理解包括氧化应激和炎症的中心作用。通过循环生物标志物或成像技术识别这些过程可能有助于早期诊断和风险分层。此外,缓解氧化应激和炎症的治疗策略有望预防心力衰竭的发展,或至少减轻心脏损伤,尽管需要进一步的证据证明其疗效,无论是单独治疗还是与神经激素拮抗剂(目前采用的标准)联合治疗。

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