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Comprehensive validation of cardiovascular magnetic resonance techniques for the assessment of myocardial extracellular volume

机译:心血管磁共振技术用于评估心肌细胞外容量的全面验证

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Background: Extracellular matrix expansion is a key element of ventricular remodeling and a potential therapeutic target. Cardiovascular magnetic resonance (CMR) T1-mapping techniques are increasingly used to evaluate myocardial extracellular volume (ECV); however, the most widely applied methods are without histological validation. Our aim was to perform comprehensive validation of (1) dynamic-equilibrium CMR (DynEq-CMR), where ECV is quantified using hematocrit-adjusted myocardial and blood T1 values measured before and after gadolinium bolus; and (2) isolated measurement of myocardial T1, used as an ECV surrogate. Methods and Results: Whole-heart histological validation was performed using 96 tissue samples, analyzed for picrosirius red collagen volume fraction, obtained from each of 16 segments of the explanted hearts of 6 patients undergoing heart transplantation who had prospectively undergone CMR before transplantation (median interval between CMR and transplantation, 29 days). DynEq-CMR-derived ECV was calculated from T 1 measurements made using a modified Look-Locker inversion recovery sequence before and 10 and 15 minutes post contrast. In addition, ECV was measured 2 to 20 minutes post contrast in 30 healthy volunteers. There was a strong linear relationship between DynEq-CMR-derived ECV and histological collagen volume fraction (P0.001; within-subject: r=0.745; P0.001; r2=0.555 and betweensubject: r=0.945; P0.01; r2=0.893; for ECV calculated using 15-minute postcontrast T1). Correlation was maintained throughout the entire heart. Isolated postcontrast T1 measurement showed significant within-subject correlation with histological collagen volume fraction (r=-0.741; P0.001; r2=0.550 for 15-minute postcontrast T1), but between-subject correlations were not significant. DynEq-CMR-derived ECV varied significantly according to contrast dose, myocardial region, and sex. Conclusions: DynEq-CMR-derived ECV shows a good correlation with histological collagen volume fraction throughout the whole heart. Isolated postcontrast T1 measurement is insufficient for ECV assessment.
机译:背景:细胞外基质扩张是心室重构的关键因素,也是潜在的治疗靶点。越来越多地使用心血管磁共振(CMR)T1映射技术来评估心肌细胞外体积(ECV)。但是,应用最广泛的方法未经组织学验证。我们的目的是对(1)动态平衡CMR(DynEq-CMR)进行全面验证,其中,使用oc剂量推注前后测得的血细胞比容调整后的心肌和血液T1值对ECV进行量化; (2)单独测量心肌T1,用作ECV替代指标。方法和结果:使用96份组织样本进行全心组织学验证,分析皮索里乌斯红胶原的体积分数,该样本取自6例接受心脏移植的患者在移植前接受CMR的16例离体心脏中的每一个(中位间隔)在CMR和移植之间(29天)。 DynEq-CMR衍生的ECV由T 1测量得出,该测量在对比之前,对比之后10和15分钟使用改良的Look-Locker反转恢复序列进行。此外,在30位健康志愿者的对比后2至20分钟测量了ECV。 DynEq-CMR衍生的ECV与组织胶原蛋白体积分数之间存在很强的线性关系(P <0.001;受试者内部:r = 0.745; P <0.001; r2 = 0.555;受试者之间:r = 0.945; P <0.01; r2 = 0.893;对于使用15分钟对比后T1计算的ECV)。整个心脏都保持了相关性。单独的对比后T1测量显示受试者内部与组织学胶原蛋白体积分数具有显着相关性(对比15分钟后T1,r = -0.741; P <0.001; r2 = 0.550),但受试者间相关性不显着。根据对比剂量,心肌区域和性别,DynEq-CMR衍生的ECV差异很大。结论:DynEq-CMR衍生的ECV与整个心脏的组织学胶原蛋白体积分数具有良好的相关性。孤立的造影剂T1测量不足以进行ECV评估。

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