Feature tracking CMR reveals abnormal strain in preclinical arrhythmogenic right ventricular dysplasia/ cardiomyopathy : A multisoftware feasibility and clinical implementation study

Aliyari Ghasebeh, Mounes; Bluemke, David A.; Bourfiss, M; Calkins, Hugh; James, Cynthia A.; Kamel, Ihab R.; Mohamed Hoesein, Firdaus A.; Murray, Brittney; Tandri, Harikrishna; Te Riele, Anneline S.J.M.; Tichnell, Crystal; Velthuis, Birgitta K.; Vigneault, Davis M; Zimmerman, Stefan L.

Feature tracking CMR reveals abnormal strain in preclinical arrhythmogenic right ventricular dysplasia/ cardiomyopathy : A multisoftware feasibility and clinical implementation study

Authors: Mounes Aliyari Ghasebeh
David A. Bluemke
M Bourfiss
Hugh Calkins
Cynthia A. James
Ihab R. Kamel
Firdaus A. Mohamed Hoesein
Brittney Murray
Harikrishna Tandri
Anneline S.J.M. Te Riele
Crystal Tichnell
Birgitta K. Velthuis
Davis M Vigneault
Stefan L. Zimmerman
Publication date: 1 September 2017
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Abstract

Background: Regional right ventricular (RV) dysfunction is the hallmark of Arrhythmogenic Right Ventricular Dysplasia/Cardiomyopathy (ARVD/C), but is currently only qualitatively evaluated in the clinical setting. Feature Tracking Cardiovascular Magnetic Resonance (FT-CMR) is a novel quantitative method that uses cine CMR to calculate strain values. However, most prior FT-CMR studies in ARVD/C have focused on global RV strain using different software methods, complicating implementation of FT-CMR in clinical practice. We aimed to assess the clinical value of global and regional strain using FT-CMR in ARVD/C and to determine differences between commercially available FT-CMR software packages. Methods: We analyzed cine CMR images of 110 subjects (39 overt ARVD/C [mutation+/phenotype+], 40 preclinical ARVD/C [mutation+/phenotype-] and 31 control) for global and regional (subtricuspid, anterior, apical) RV strain in the horizontal longitudinal axis using four FT-CMR software methods (Multimodality Tissue Tracking, TomTec, Medis and Circle Cardiovascular Imaging). Intersoftware agreement was assessed using Bland Altman plots. Results: For global strain, all methods showed reduced strain in overt ARVD/C patients compared to control subjects (p 0.275). For regional strain, overt ARVD/C patients showed reduced strain compared to control subjects in all segments which reached statistical significance in the subtricuspid region for all software methods (p < 0.037), in the anterior wall for two methods (p < 0.005) and in the apex for one method (p = 0.012). Preclinical subjects showed abnormal subtricuspid strain compared to control subjects using one of the software methods (p = 0.009). Agreement between software methods for absolute strain values was low (Intraclass Correlation Coefficient = 0.373). Conclusions: Despite large intersoftware variability of FT-CMR derived strain values, all four software methods distinguished overt ARVD/C patients from control subjects by both global and subtricuspid strain values. In the subtricuspid region, one software package distinguished preclinical from control subjects, suggesting the potential to identify early ARVD/C prior to overt disease expression

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