Increased cardiac involvement in Fabry disease using blood-corrected native T1 mapping

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作者
Jannike Nickander
Ben Cole
Sabrina Nordin
Ravi Vijapurapu
Richard P. Steeds
James C. Moon
Peter Kellman
Martin Ugander
Rebecca Kozor
机构
[1] Karolinska University Hospital,Department of Clinical Physiology
[2] and Karolinska Institutet,Kolling Institute
[3] Royal North Shore Hospital,Institute of Cardiovascular Science
[4] and University of Sydney,Institute of Cardiovascular Science
[5] University College London,Charles Perkins Center, Faculty of Medicine and Health
[6] University of Birmingham,Sydney Medical School
[7] National Heart,undefined
[8] Lung,undefined
[9] and Blood Institute,undefined
[10] National Institutes of Health,undefined
[11] University of Sydney,undefined
[12] Royal North Shore Hospital,undefined
[13] North Shore Private Hospital,undefined
[14] University of Sydney,undefined
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摘要
Fabry disease (FD) is a rare lysosomal storage disorder resulting in myocardial sphingolipid accumulation which is detectable by cardiovascular magnetic resonance as low native T1. However, myocardial T1 contains signal from intramyocardial blood which affects variability and consequently measurement precision and accuracy. Correction of myocardial T1 by blood T1 increases precision. We therefore deployed a multicenter study of FD patients (n = 218) and healthy controls (n = 117) to investigate if blood-correction of myocardial native T1 increases the number of FD patients with low T1, and thus reclassifies FD patients as having cardiac involvement. Cardiac involvement was defined as a native T1 value 2 standard deviations below site-specific means in healthy controls for both corrected and uncorrected measures. Overall low T1 was 135/218 (62%) uncorrected vs. 145/218 (67%) corrected (p = 0.02). With blood-correction, 13/83 previously normal patients were reclassified to low T1. This reclassification appears clinically relevant as 6/13 (46%) of reclassified had focal late gadolinium enhancement or left ventricular hypertrophy as signs of cardiac involvement. Blood-correction of myocardial native T1 increases the proportion of FD subjects with low myocardial T1, with blood-corrected results tracking other markers of cardiac involvement. Blood-correction may potentially offer earlier detection and therapy initiation, but merits further prospective studies.
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