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Effect of myocardial dysfunction in cardiac morbidity and all cause mortality in childhood cancer subjects treated with anthracycline therapy

机译:蒽环类药物治疗的儿童癌症患者心肌功能障碍对心脏发病率和所有原因死亡率的影响

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Background Subacute cardiotoxicity, consisting of acute myocyte damage and associated left ventricular dysfunction, occurs early during anthracycline therapy. We investigated the impact of myocardial dysfunction, defined herein by a shortening fraction (SF)? Methods Five hundred thirty-one childhood cancer survivors exposed to anthracyclines were enrolled and studied on average 10 (1.4–27.3) years following their initial exposure. The medical records were reviewed to identify known risk factors associated with cardiotoxicity, including cumulative anthracycline dose, length of post-therapy interval, administration of other cardiotoxic medications (vinca alkaloids), previous heart disease, radiation dose to the heart, history of bone marrow transplantation, age at treatment, gender, systolic dysfunction, and history of congestive heart failure during anthracycline therapy. Results Ninety subjects (16.9 %) developed SF?2. The all-cause mortality ratio was almost seven-fold higher (95 % CI, 2.40-fold to 17.81-fold higher) if a subject developed systolic dysfunction, defined by a previous SF? Conclusions This study demonstrates an almost seven-fold increase in all cause mortality in pediatric cancer survivors with a history of anthracycline induced myocardial dysfunction defined as SF
机译:背景在蒽环类药物治疗的早期,亚急性心脏毒性包括急性心肌细胞损伤和相关的左心室功能障碍。我们调查了心肌功能障碍的影响,本文通过缩短分数(SF)来定义?方法招募了513名暴露于蒽环类药物的儿童期癌症幸存者,并在首次暴露后平均10年(1.4–27.3)年进行了研究。对病历进行了审查,以确定与心脏毒性有关的已知危险因素,包括累积蒽环类药物剂量,治疗间隔时间,其他心脏毒性药物(长春花生物碱)的使用,先前的心脏病,心脏的放射剂量,骨髓病史移植,治疗年龄,性别,收缩功能障碍以及蒽环类药物治疗期间充血性心力衰竭的病史。结果90名受试者(16.9%)出现了SF?2 。如果受试者出现由先前的SF?定义的收缩功能障碍,则全因死亡率几乎高出七倍(95%CI,高2.40倍至17.81倍)。结论这项研究表明,有蒽环类药物史的被定义为SF的小儿癌症幸存者的全因死亡率几乎增加了7倍

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