Measuring cardiomyocyte cellular characteristics in cardiac hypertrophy using diffusion‐weighted MRI

Author:

Farzi Mohsen1ORCID,Coveney Sam1ORCID,Afzali Maryam12ORCID,Zdora Marie‐Christine34,Lygate Craig A.5ORCID,Rau Christoph3,Frangi Alejandro F.6ORCID,Dall'Armellina Erica1ORCID,Teh Irvin1ORCID,Schneider Jürgen E.1ORCID

Affiliation:

1. Biomedical Imaging Science Department, Leeds Institute of Cardiovascular and Metabolic Medicine University of Leeds Leeds UK

2. Cardiff University Brain Research Imaging Centre (CUBRIC), School of Psychology Cardiff University Cardiff UK

3. Diamond Light Source Ltd. Harwell Science and Innovation Campus Didcot UK

4. Department of Physics & Astronomy University College London London UK

5. Division of Cardiovascular Medicine, Radcliffe Department of Medicine University of Oxford Oxford UK

6. Centre for Computational Imaging and Simulation Technologies in Biomedicine (CISTIB), School of Computing University of Leeds Leeds UK

Abstract

PurposeThis paper presents a hierarchical modeling approach for estimating cardiomyocyte major and minor diameters and intracellular volume fraction (ICV) using diffusion‐weighted MRI (DWI) data in ex vivo mouse hearts.MethodsDWI data were acquired on two healthy controls and two hearts 3 weeks post transverse aortic constriction (TAC) using a bespoke diffusion scheme with multiple diffusion times (), q‐shells and diffusion encoding directions. Firstly, a bi‐exponential tensor model was fitted separately at each diffusion time to disentangle the dependence on diffusion times from diffusion weightings, that is, b‐values. The slow‐diffusing component was attributed to the restricted diffusion inside cardiomyocytes. ICV was then extrapolated at using linear regression. Secondly, given the secondary and the tertiary diffusion eigenvalue measurements for the slow‐diffusing component obtained at different diffusion times, major and minor diameters were estimated assuming a cylinder model with an elliptical cross‐section (ECS). High‐resolution three‐dimensional synchrotron X‐ray imaging (SRI) data from the same specimen was utilized to evaluate the biophysical parameters.ResultsEstimated parameters using DWI data were (control 1/control 2 vs. TAC 1/TAC 2): major diameter—17.4 m/18.0 m versus 19.2 m/19.0 m; minor diameter—10.2 m/9.4 m versus 12.8 m/13.4 m; and ICV—62%/62% versus 68%/47%. These findings were consistent with SRI measurements.ConclusionThe proposed method allowed for accurate estimation of biophysical parameters suggesting cardiomyocyte diameters as sensitive biomarkers of hypertrophy in the heart.

Funder

Royal Academy of Engineering

British Heart Foundation

Wellcome Trust

Publisher

Wiley

Subject

Radiology, Nuclear Medicine and imaging

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