基于磁共振成像的连续监测用于诊断蒽环类药物诱导的心脏毒性的早期阶段。
Serial Magnetic Resonance Imaging to Identify Early Stages of Anthracycline-Induced Cardiotoxicity.
机构信息
Centro Nacional de Investigaciones Cardiovasculares (CNIC), Madrid, Spain; Centro de Investigación Biomédica en Red en Enfermedades Cardiovasculares (CIBERCV), Madrid, Spain.
Centro Nacional de Investigaciones Cardiovasculares (CNIC), Madrid, Spain; Complejo Hospitalario Ruber Juan Bravo, Madrid, Spain.
出版信息
J Am Coll Cardiol. 2019 Feb 26;73(7):779-791. doi: 10.1016/j.jacc.2018.11.046.
BACKGROUND
Anthracycline-induced cardiotoxicity is a major clinical problem, and early cardiotoxicity markers are needed.
OBJECTIVES
The purpose of this study was to identify early doxorubicin-induced cardiotoxicity by serial multiparametric cardiac magnetic resonance (CMR) and its pathological correlates in a large animal model.
METHODS
Twenty pigs were included. Of these, 5 received 5 biweekly intracoronary doxorubicin doses (0.45 mg/kg/injection) and were followed until sacrifice at 16 weeks. Another 5 pigs received 3 biweekly doxorubicin doses and were followed to 16 weeks. A third group was sacrificed after the third dose. All groups underwent weekly CMR examinations including anatomical and T and T mapping (including extracellular volume [ECV] quantification). A control group was sacrificed after the initial CMR.
RESULTS
The earliest doxorubicin-cardiotoxicity CMR parameter was T relaxation-time prolongation at week 6 (2 weeks after the third dose). T mapping, ECV, and left ventricular (LV) motion were unaffected. At this early time point, isolated T prolongation correlated with intracardiomyocyte edema secondary to vacuolization without extracellular space expansion. Subsequent development of T mapping and ECV abnormalities coincided with LV motion defects: LV ejection fraction declined from week 10 (2 weeks after the fifth and final doxorubicin dose). Stopping doxorubicin therapy upon detection of T prolongation halted progression to LV motion deterioration and resolved intracardiomyocyte vacuolization, demonstrating that early T prolongation occurs at a reversible disease stage.
CONCLUSIONS
T mapping during treatment identifies intracardiomyocyte edema generation as the earliest marker of anthracycline-induced cardiotoxicity, in the absence of T mapping, ECV, or LV motion defects. The occurrence of these changes at a reversible disease stage shows the clinical potential of this CMR marker for tailored anthracycline therapy.
背景
蒽环类药物诱导的心脏毒性是一个主要的临床问题,需要早期心脏毒性标志物。
目的
本研究旨在通过连续多参数心脏磁共振(CMR)及其在大型动物模型中的病理相关性,来确定多柔比星早期诱导的心脏毒性。
方法
共纳入 20 头猪,其中 5 头接受 5 次双周冠状动脉内多柔比星剂量(0.45mg/kg/次),并在 16 周时处死。另外 5 头猪接受 3 次双周多柔比星剂量,并随访至 16 周。第三组在第三次剂量后处死。所有组均进行每周一次的 CMR 检查,包括解剖和 T 和 T 映射(包括细胞外容积[ECV]定量)。对照组在初次 CMR 后处死。
结果
最早的多柔比星心脏毒性 CMR 参数是 T 弛豫时间延长,发生在第 6 周(第三次剂量后 2 周)。T 映射、ECV 和左心室(LV)运动均不受影响。在这个早期时间点,孤立的 T 延长与心肌细胞水肿有关,继发于空泡化而没有细胞外空间扩张。随后 T 映射和 ECV 异常的发展与 LV 运动缺陷同时发生:LV 射血分数从第 10 周(第五次和最后一次多柔比星剂量后 2 周)开始下降。在检测到 T 延长时停止多柔比星治疗,阻止了 LV 运动恶化的进展,并解决了心肌细胞空泡化,表明早期 T 延长发生在可逆转的疾病阶段。
结论
治疗期间的 T 映射可识别心肌细胞水肿的产生作为蒽环类药物诱导的心脏毒性的最早标志物,在没有 T 映射、ECV 或 LV 运动缺陷的情况下。这些变化在可逆转的疾病阶段发生表明了这种 CMR 标志物在定制蒽环类药物治疗中的临床潜力。
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