MicroRNA Induced Cardiac Reprogramming In Vivo

Author:

Jayawardena Tilanthi M.1,Finch Elizabeth A.1,Zhang Lunan1,Zhang Hengtao1,Hodgkinson Conrad P.1,Pratt Richard E.1,Rosenberg Paul B.1,Mirotsou Maria1,Dzau Victor J.1

Affiliation:

1. From the Mandel Center for Hypertension Research (T.M.J., L.Z., C.P.H., R.E.P., M.M., V.J.D.) and the Ion Channel Research Unit (E.A.F., H.Z., P.B.R.), Division of Cardiovascular Medicine, Department of Medicine, Duke University Medical Center, Durham, NC; and Sarah Steadman Nutrition and Metabolism Center, Duke University Medical Center, Durham, NC (P.B.R.).

Abstract

Rationale : A major goal for the treatment of heart tissue damaged by cardiac injury is to develop strategies for restoring healthy heart muscle through the regeneration and repair of damaged myocardium. We recently demonstrated that administration of a specific combination of microRNAs (miR combo) into the infarcted myocardium leads to direct in vivo reprogramming of noncardiac myocytes to cardiac myocytes. However, the biological and functional consequences of such reprogramming are not yet known. Objective : The aim of this study was to determine whether noncardiac myocytes directly reprogrammed using miRNAs in vivo develop into mature functional cardiac myocytes in situ, and whether reprogramming leads to improvement of cardiac function. Methods and Results : We subjected fibroblast-specific protein 1-Cre mice/tandem dimer Tomato (tdTomato) mice to cardiac injury by permanent ligation of the left anterior descending coronary artery and injected lentiviruses encoding miR combo or a control nontargeting miRNA. miR combo significantly increased the number of reprogramming events in vivo. Five to 6 weeks after injury, morphological and physiological properties of tdTomato and tdTomato + cardiac myocyte–like cells were analyzed ex vivo. tdTomato + cells expressed cardiac myocyte markers, sarcomeric organization, excitation–contraction coupling, and action potentials characteristic of mature ventricular cardiac myocytes (tdTomato cells). Reprogramming was associated with improvement of cardiac function, as analyzed by serial echocardiography. There was a time delayed and progressive improvement in fractional shortening and other measures of ventricular function, indicating that miR combo promotes functional recovery of damaged myocardium. Conclusions : The findings from this study further validate the potential use of miRNA-mediated reprogramming as a therapeutic approach to promote cardiac regeneration after myocardial injury.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine,Physiology

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