Right ventricular cardiomyocyte expansion accompanies cardiac regeneration in newborn mice after large left ventricular infarcts
Tianyuan Hu, Mona Malek Mohammadi, Fabian Ebach, Michael Hesse, Michael I. Kotlikoff, Bernd K. Fleischmann
Tianyuan Hu, Mona Malek Mohammadi, Fabian Ebach, Michael Hesse, Michael I. Kotlikoff, Bernd K. Fleischmann
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Research Article Cardiology

Right ventricular cardiomyocyte expansion accompanies cardiac regeneration in newborn mice after large left ventricular infarcts

Abstract

Cauterization of the root of the left coronary artery (LCA) in the neonatal heart on postnatal day 1 (P1) resulted in large, reproducible lesions of the left ventricle (LV), and an attendant marked adaptive response in the right ventricle (RV). The response of both chambers to LV myocardial infarction involved enhanced cardiomyocyte (CM) division and binucleation, as well as LV revascularization, leading to restored heart function within 7 days post surgery (7 dps). By contrast, infarction of P3 mice resulted in cardiac scarring without a significant regenerative and adaptive response of the LV and the RV, leading to subsequent heart failure and death within 7 dps. The prominent RV myocyte expansion in P1 mice involved an acute increase in pulmonary arterial pressure and a unique gene regulatory response, leading to an increase in RV mass and preserved heart function. Thus, distinct adaptive mechanisms in the RV, such as CM proliferation and RV expansion, enable marked cardiac regeneration of the infarcted LV at P1 and full functional recovery.

Authors

Tianyuan Hu, Mona Malek Mohammadi, Fabian Ebach, Michael Hesse, Michael I. Kotlikoff, Bernd K. Fleischmann

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Figure 4

CM cytokinesis and binucleation strongly increase in the LV of P1, but not of P3, MI hearts.

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CM cytokinesis and binucleation strongly increase in the LV of P1, but n...
(A and B) Images (A) and quantitation (B) of MKI67+ CMs in LV marked by costaining for MKI67, TNNI3, and with DAPI. Scale bar: 20 μm. (C) Mosaic images of LV heart sections of CAG-eGFP-anillin mice costained for eGFP and TNNI3; arrowheads mark eGFP+ CMs, which are shown at higher magnification (×5.5) as confocal images in insets. Scale bar: 20 μm. (D) Quantitation of eGFP+ CMs in the LV. (EG) Cytokinetic and binucleating CMs in heart sections costained for eGFP, AURKB, TNNI3, and with DAPI; midbodies were identified based on costaining for eGFP and AURKB (arrows). Two-sided arrows mark the distance between the 2 nuclei in the same CM; typical (yellow arrows) or atypical midbody location (green arrows) mark cytokinetic (F) and binucleating (G) CMs. Scale bar: 10 μm. (H) Images of mono- and binucleated CMs isolated from αMHC-H2BmCherry hearts at P5. Scale bar: 20 μm. (I) Quantitation of the percentage of binucleated/total CMs isolated from whole hearts. *P < 0.05; **P < 0.01; ***P < 0.001; ****P < 0.0001 by 1-way ANOVA with Holm-Šidák post hoc test. NS, no significance.