Subcellular remodelling may induce cardiac dysfunction in congestive heart failure

doi:10.1093/cvr/cvn281

Cardiovascular Research Advance Access originally published online on October 13, 2008
Cardiovascular Research 2009 81(3):429-438; doi:10.1093/cvr/cvn281

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Subcellular remodelling may induce cardiac dysfunction in congestive heart failure

Naranjan S. Dhalla^*, Harjot K. Saini-Chohan, Delfin Rodriguez-Leyva, Vijayan Elimban, Melissa R. Dent and Paramjit S. Tappia

Institute of Cardiovascular Sciences, St Boniface General Hospital Research Centre, Department of Physiology, Faculty of Medicine, University of Manitoba, 351 Tache Avenue, Winnipeg, Manitoba, Canada R2H 2A6

^* Corresponding author. Tel: +1 204 235 3417; fax: +1 204 237-0347. E-mail address: nsdhalla{at}sbrc.ca

It is commonly held that cardiac remodelling, represented bychanges in muscle mass, size, and shape of the heart, explainsthe progression of congestive heart failure (CHF). However,this concept does not provide any clear information regardingthe development of cardiac dysfunction in CHF. Extensive researchhas revealed that various subcellular organelles such as theextracellular matrix, sarcolemma, sarcoplasmic reticulum, myofibrils,mitochondria, and nucleus undergo varying degrees of changesin their biochemical composition and molecular structure inCHF. This subcellular remodelling occurs due to alterationsin cardiac gene expression as well as activation of differentproteases and phospholipases in the failing hearts. Severalmechanisms including increased ventricular wall stress, prolongedactivation of the renin–angiotensin and sympathetic systems,and oxidative stress have been suggested to account for subcellularremodelling in CHF. Furthermore, subcellular remodelling isassociated with changes in cardiomyocyte structure, cation homeostasisas well as functional activities of cation channels and transporters,receptor-mediated signal transduction, Ca²⁺-cycling proteins,contractile and regulatory proteins, and energy production duringthe development of heart failure. The existing evidence supportsthe view that subcellular remodelling may result in cardiacdysfunction and thus play a critical role in the transitionof cardiac hypertrophy to heart failure.

KEYWORDS Cardiac hypertrophy; Heart failure; Sarcolemmal remodelling; Sarcoplasmic reticular remodelling; Myofibrillar remodelling; Mitochondrial remodelling; Extracellular remodelling

Time for primary review: 32 days

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