人心脏型脂肪酸结合蛋白作为阿霉素心脏毒性的早期诊断标志物

A. Elghandour, M. E. Sorady, S. Azab, M. Elrahman
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引用次数: 31

摘要

非霍奇金淋巴瘤(NHL)患者接受多柔比星化疗后的进行性心脏毒性可能导致晚发性心肌病。因此,对毒性的早期预测可以预防这些患者的心力衰竭。这项工作的目的是研究H-FABP作为蒽环类药物引起的心脏毒性的早期诊断标志物的作用,以及脑利钠肽(BNP)作为这类患者心室功能障碍的指示。我们的研究是在40例NHL患者中进行的,他们接受了6个周期的含阿霉素化疗方案(CHOP),不超过阿霉素的总允许剂量(500mg /m2)。我们的研究纳入了10名健康对照。人心脏型脂肪酸结合蛋白(H-FABP)在CHOP第一个周期后24小时测定。在化疗开始前和CHOP最后一个周期后测定血浆BNP水平。静息超声心动图也在化疗周期之前和结束时进行。我们的8例患者的射血分数(EF)在第六个周期结束时降至50%以下。EF低于50%的患者H-FABP和BNP均升高,且两者呈正相关。我们的结论是,H-FABP可以作为预测阿霉素引起的心肌病的可靠的早期标志物。因此,对于H-FABP升高的患者,可以考虑无心脏毒性的替代治疗方式,以防止这些患者随后的心力衰竭。
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Human heart-type fatty acid-binding protein as an early diagnostic marker of doxorubicin cardiac toxicity
Progressive cardiotoxicity following treatment with doxorubicin-based chemotherapy in patients with non-Hodgkin's lymphoma (NHL) may lead to late onset cardiomyopathy. So, early prediction of toxicity can lead to prevention of heart failure in these patients. The aim of this work was to investigate the role of H-FABP as an early diagnostic marker of anthracycline-induced cardiac toxicity together with brain natriuretic peptide (BNP) as an indication of ventricular dysfunction in such patients. Our study was conducted on 40 NHL patients who received 6 cycles of a doxorubicin containing chemotherapy protocol (CHOP), not exceeding the total allowed dose of doxorubicin (500 mg/m2). Ten healthy controls were included in our study. Human heart-type fatty acid-binding protein (H-FABP) was assessed 24 hours after the first cycle of CHOP. Plasma levels of BNP were estimated both before starting chemotherapy and after the last cycle of CHOP. Resting echocardiography was also performed before and at the end of chemotherapy cycles. The ejection fraction (EF) of 8 of our patients decreased below 50% at the end of the sixth cycle. Elevated levels of both H-FABP and BNP were found in all patients wth EF below 50% and both markers showed a positive correlation with each other. We concluded that H-FABP may serve as a reliable early marker for prediction of cardiomyopathy induced by doxorubicin. Thus, in patients with elevated H-FABP, alternative treatment modalities with no cardiac toxicity may be considered in order to prevent subsequent heart failure in these patients.
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