Characterization of myocardial fiber orientation to assess therapeutic exosomes from cardiosphere-derived cells (CDCs) in myocardial infarcted porcine with in vivo diffusion-tensor CMR on a clinical scanner

Background Diffusion-Tensor cardiovascular magnetic resonance (DT-CMR) is capable of mapping myocardial fiber orientation [1,2]. It has been demonstrated in myocardial infarction (MI) murine models that DT-CMR can identify the effects of stem cell therapy on myocardial fiber orientation [3]. However, it remains to be seen if this recent work is translatable to large animal and clinical studies. We propose the application of a well-established in vivo cardiac DT-CMR technique [4] to characterize myocardial fiber orientation before and after the novel regenerative therapy of using intramyocardial injection of exosomes from cardiosphere-derived cells (CDCs) in a MI porcine model.

Characterization of myocardial fiber orientation to assess therapeutic exosomes from cardiospherederived cells (CDCs) in myocardial infarcted porcine with in vivo diffusion-tensor CMR on a clinical scanner Background Diffusion-Tensor cardiovascular magnetic resonance (DT-CMR) is capable of mapping myocardial fiber orientation [1,2]. It has been demonstrated in myocardial infarction (MI) murine models that DT-CMR can identify the effects of stem cell therapy on myocardial fiber orientation [3]. However, it remains to be seen if this recent work is translatable to large animal and clinical studies. We propose the application of a well-established in vivo cardiac DT-CMR technique [4] to characterize myocardial fiber orientation before and after the novel regenerative therapy of using intramyocardial injection of exosomes from cardiosphere-derived cells (CDCs) in a MI porcine model.

Methods
MI was induced in 7 Yucatan mini pigs by balloon occlusion of the mid-LAD for 2.5 hours. The MI was allowed to heal for 4 weeks for all pigs defining baseline. Group 1 (N = 4) were treated with exosome proteins derived from CDCs. Group 2 was given a placebo.
CMR was performed at baseline and 4 weeks after treatment on a 3T Siemens Verio with the following: whole-heart 2D multi-slice (WH) morphological CMR, WH function CINE CMR, 3 short axis slice DT-CMR (STEAM, 6 dir, b = 350 s/mm 2 , 8 avg, 2 avg/BH), and WH viability CMR (LGE PSIR, TI = 315 ms). Viability and function CMR yielded scar size (SS) and ejection fraction (EF) [5], respectively. For in vivo DT-CMR, mean diffusivity (MD), fractional anisotropy (FA), and helix angle (HA) maps were calculated. HA transmurality slope (HATS) was calculated by radially sampling the transmural HA along 36 chords and fitting the slope of a linear regression between HA and transmural depth.
Wilcoxon signed-rank test was performed to evaluate the difference between mean slice values (G1 N = 12, G2 N = 9) before and after treatment (p < 0.017 significance). Change (Δ) in MD, FA, and HATS were correlated (R^2) with ΔSS and ΔEF.

Conclusions
In a MI porcine model, in vivo DT-CMR revealed that myocardial fiber orientation was preserved with CDCderived exosome treatment and adversely changed with placebo treatment consistent with observed viability and function changes. Furthermore, changes in helix transmurality highly correlated with changes in viability and function.
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