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Altered left ventricular longitudinal diastolic function correlates with reduced systolic function immediately after anthracycline chemotherapy

机译:蒽环类药物化疗后,左室纵向舒张功能改变与收缩功能降低相关

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AimsThe benefits from anthracycline chemotherapy are undermined by potentially life-threatening cardiotoxicity. Transthoracic echocardiography is the most commonly used method for monitoring cardiotoxicity, and centres on the measurement of left ventricular systolic function. The aim of this study was to utilize two-dimensional speckle tracking echocardiography (2DSTE) at baseline and immediately after anthracycline chemotherapy to investigate whether patients with significant changes in systolic function after anthracycline therapy would also develop alterations in diastolic parameters.Methods and resultsFifty-two women with histologically confirmed breast cancer were prospectively recruited. Echocardiograms were performed 1 week prior to and 1 week following chemotherapy (always before adjuvant trastuzumab or thoracic radiotherapy). Conventional Doppler, tissue velocity imaging (TVI), and 2DSTE were used to measure diastolic function. 2DSTE measurements included longitudinal diastolic strain, early (E-Sr), and late (A-Sr) myocardial strain rate. 2DSTE and left ventricular ejection fraction (LVEF) were used to measure longitudinal systolic function. Altered LV diastolic function (including E-Sr) was observed in the entire cohort after chemotherapy, with a differential reduction in participants with a post therapy LVEF <55%. Pre-chemotherapy systolic strain was found to predict reduced E-Sr post therapy (P = 0.04). Univariate predictors of E-Sr were LVEF post therapy (P = 0.049) and systolic strain post-therapy (P = 0.01). In a multivariate analysis, systolic strain after chemotherapy was the strongest independent predictor (P = 0.001).ConclusionAltered LV diastolic function was observed immediately after the administration of therapeutic doses of anthracycline chemotherapy. Furthermore, our analysis indicates that the changes in diastolic function are associated with reduced systolic function.
机译:目的潜在危及生命的心脏毒性损害了蒽环类药物化疗的益处。经胸超声心动图检查是最常用的监测心脏毒性的方法,其重点是测量左心室收缩功能。这项研究的目的是在基线和蒽环类药物化疗后立即使用二维散斑跟踪超声心动图(2DSTE),以调查蒽环类药物治疗后收缩功能有明显变化的患者是否也会产生舒张参数的改变。方法和结果52经组织学证实为乳腺癌的女性是前瞻性招募的。超声心动图是在化疗前1周和化疗后1周(总是在辅助曲妥珠单抗或胸腔放疗之前)进行的。常规多普勒,组织速度成像(TVI)和2DSTE用于测量舒张功能。 2DSTE测量包括纵向舒张应变,早期(E-Sr)和晚期(A-Sr)心肌应变率。 2DSTE和左心室射血分数(LVEF)用于测量纵向收缩功能。在整个队列研究中观察到化疗后LV舒张功能改变(包括E-Sr),治疗后LVEF <55%的参与者差异减少。发现化疗前的收缩期应变可预测治疗后E-Sr降低(P = 0.04)。 E-Sr的单因素预测因素是治疗后LVEF(P = 0.049)和治疗后收缩期应变(P = 0.01)。在多变量分析中,化疗后的收缩压是最强的独立预测因子(P = 0.001)。结论蒽环类药物化疗后立即观察到左室舒张功能改变。此外,我们的分析表明舒张功能的改变与收缩功能降低有关。

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