Atrophied Cardiomyocytes and Their Potential for Rescue and Recovery of Ventricular Function

Overview

Journal Heart Fail Rev

Date 2016 Feb 14

PMID 26872676

Citations 7

Authors

Mark R Heckle

David M Flatt

Yao Sun

Salvatore Mancarella

Tony N Marion

Ivan C Gerling

Karl T Weber

Affiliations

Soon will be listed here.

Abstract

Cardiomyocytes must be responsive to demands placed on the heart's contractile work as a muscular pump. In turn, myocyte size is largely dependent on the workload they perform. Both hypertrophied and atrophic myocytes are found in the normal and diseased ventricle. Individual myocytes become atrophic when encumbered by fibrillar collagen, such as occurs at sites of fibrosis. The mechanisms include: (a) being immobilized and subject to disuse with ensuing protein degradation mediated by redox-sensitive, proteolytic ligases of the ubiquitin-proteasome system and (b) dedifferentiated re-expressing fetal genes induced by low intracellular triiodothyronine (T3) via thyroid hormone receptor β1. This myocyte-selective, low T3 state is a consequence of heterocellular signaling emanating from juxtaposed scar tissue myofibroblasts and their secretome with its de novo generation of angiotensin II. In a paracrine manner, angiotensin II promotes myocyte Ca(2+) entry and subsequent Ca(2+) overload with ensuing oxidative stress that overwhelms antioxidant defenses to activate deiodinase-3 and its enzymatic degradation of T3. In the failing heart, atrophic myocytes represent an endogenous population of viable myocytes which could be rescued to augment contractile mass, reduce systolic wall stress (afterload) and recover ventricular function. Experimental studies have shown the potential for the rescue and recovery of atrophic myocytes in rebuilding the myocardium--a method complementary to today's quest in regenerating myocardium using progenitor cells.

Citing Articles

Sex-Linked Differences in Cardiac Atrophy After Heterotopic Heart Transplantation: No Direct Relation to the Actions of Sex Steroid Hormones.

Kolesar D, Kujal P, Mrazova I, Pokorny M, Skaroupkova P, Vanourkova Z Physiol Res. 2024; 73(S2):S527-S539.

PMID: 39589301 PMC: 11627268.

Sex-Linked Differences in Cardiac Atrophy After Mechanical Unloading Induced by Heterotopic Heart Transplantation.

Kolesar D, Kujal P, Mrazova I, Pokorny M, Skaroupkova P, Sadowski J Physiol Res. 2024; 73(1):9-25.

PMID: 38466001 PMC: 11019613. DOI: 10.33549/physiolres.935217.

Distinct Cardiac Connexin-43 Expression in Hypertrophied and Atrophied Myocardium May Impact the Vulnerability of the Heart to Malignant Arrhythmias. A Pilot Study.

Szeiffova Bacova B, Andelova K, Sykora M, T E, Kurahara L, Slezak J Physiol Res. 2023; 72(S1):S37-S45.

PMID: 37294117 PMC: 10292813. DOI: 10.33549/physiolres.935025.

Does Myocardial Atrophy Represent Anti-Arrhythmic Phenotype?.

Szeiffova Bacova B, Andelova K, Sykora M, Benova T, Barancik M, Kurahara L Biomedicines. 2022; 10(11).

PMID: 36359339 PMC: 9687767. DOI: 10.3390/biomedicines10112819.

Intersection of the Ubiquitin-Proteasome System with Oxidative Stress in Cardiovascular Disease.

Qiu M, Chen J, Li X, Zhuang J Int J Mol Sci. 2022; 23(20).

PMID: 36293053 PMC: 9603077. DOI: 10.3390/ijms232012197.

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