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Abstract #1496

Cardiac Phantom-based Inter-site Calibration of T2, T1, and ECV Measurements

Carly Anne Lockard1, Ruei-yuan Tu1, Ke Yan2, Aspen Duffin2, Kimberly Crum3, Scott Auerbach4, Brian Fonseca4, Markus Renno5, Kenneth Knecht5, Margaret M Samyn2, Jonathan Soslow3, and Bruce M Damon1
1Stephens Family Clinical Research Institute, Carle Clinical Imaging Research Program, Carle Foundation Hospital, Urbana, IL, United States, 2Medical College of Wisconsin, Milwaukee, WI, United States, 3Vanderbilt University, Nashville, TN, United States, 4Children’s Hospital Colorado, Denver, CO, United States, 5Arkansas Children’s Hospital, Little Rock, AR, United States

Synopsis

Keywords: Myocardium, Heart, Transplant, T1-mapping, T2-mapping, ECV, Rejection, Calibration

Motivation: Acute rejection is the leading cause of death in pediatric heart transplant (PHTx) recipients. Endomyocardial biopsy is currently required to monitor for rejection. Quantitative cardiac magnetic resonance (CMR) is a potential non-invasive monitoring tool, with T2, T1, and ECV mapping providing information about fibrosis and edema. However, measurements vary between sites.

Goal(s): To measure inter-site/temporal variability and calibrate multisite PHTx CMR data.

Approach: We investigated manganese-chloride solution cardiac phantom T2 and T1 repeatability and inter-site variation, and impact of calibration on PHTx data.

Results: Calibration reduced inter-site variability in phantom and PHTx measurements.

Impact: Our preliminary results illustrating inter-site variation in CMR-relevant phantom T2 and T1 measurements support the need for inter-site calibration when multi-center trials are conducted using CMR parametric imaging (T2, T1, and calculated ECV).

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Keywords