Assessing heterogeneity on cardiovascular magnetic resonance imaging: a novel approach to diagnosis and risk stratification in cardiac diseases

Author:

Hesse Kerrick12ORCID,Khanji Mohammed Y234ORCID,Aung Nay24ORCID,Dabbagh Ghaith Sharaf56,Petersen Steffen E2478ORCID,Chahal C Anwar A469ORCID

Affiliation:

1. Cardiology Department, James Cook University Hospital , Marton Road, Middlesbrough TS4 3BW , UK

2. Centre for Advanced Cardiovascular Imaging, William Harvey Research Institute, NIHR Barts Biomedical Research Centre, Queen Mary University London , Charterhouse Square, London EC1M 6BQ , UK

3. Newham University Hospital, Barts Health NHS Trust , Geln Road, Plaistow, London E13 8SL , UK

4. Barts Heart Centre, Barts Health NHS Trust, St Bartholomew’s Hospital , West Smithfield, London EC1A 7BE , UK

5. Division of Cardiovascular Medicine, University of Michigan , Ann Arbor, MI , USA

6. Center for Inherited Cardiovascular Diseases, WellSpan Health , 30 Monument Road, York, PA 17403 , USA

7. Health Data Research UK , Gibbs Building, 215 Euston Road, London NW1 2BE , UK

8. Alan Turing Institute , 96 Euston Road, London NW1 2DB , UK

9. Department of Cardiovascular Medicine, Mayo Clinic , 200 First Str, SW Rochester, MN 55905 , USA

Abstract

Abstract Cardiac disease affects the heart non-uniformly. Examples include focal septal or apical hypertrophy with reduced strain in hypertrophic cardiomyopathy, replacement fibrosis with akinesia in an infarct-related coronary artery territory, and a pattern of scarring in dilated cardiomyopathy. The detail and versatility of cardiovascular magnetic resonance (CMR) imaging mean it contains a wealth of information imperceptible to the naked eye and not captured by standard global measures. CMR-derived heterogeneity biomarkers could facilitate early diagnosis, better risk stratification, and a more comprehensive prediction of treatment response. Small cohort and case–control studies demonstrate the feasibility of proof-of-concept structural and functional heterogeneity measures. Detailed radiomic analyses of different CMR sequences using open-source software delineate unique voxel patterns as hallmarks of histopathological changes. Meanwhile, measures of dispersion applied to emerging CMR strain sequences describe variable longitudinal, circumferential, and radial function across the myocardium. Two of the most promising heterogeneity measures are the mean absolute deviation of regional standard deviations on native T1 and T2 and the standard deviation of time to maximum regional radial wall motion, termed the tissue synchronization index in a 16-segment left ventricle model. Real-world limitations include the non-standardization of CMR imaging protocols across different centres and the testing of large numbers of radiomic features in small, inadequately powered patient samples. We, therefore, propose a three-step roadmap to benchmark novel heterogeneity biomarkers, including defining normal reference ranges, statistical modelling against diagnosis and outcomes in large epidemiological studies, and finally, comprehensive internal and external validations.

Funder

British Heart Foundation Clinical Research Training Fellowship

Publisher

Oxford University Press (OUP)

Subject

Cardiology and Cardiovascular Medicine,Radiology, Nuclear Medicine and imaging,General Medicine

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