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Cardiovascular Research 2003 57(4):953-960; doi:10.1016/S0008-6363(02)00768-X
© 2003 by European Society of Cardiology
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Copyright © 2003, European Society of Cardiology

Stretch-elicited Na+/H+ exchanger activation: the autocrine/paracrine loop and its mechanical counterpart

Horacio E Cingolania,*,1, Néstor G Péreza,1, Burket Pieskeb, Dirk von Lewinskib and María C Camilión de Hurtadoa,1

aCentro de Investigaciones Cardiovasculares, Facultad de Ciencias Médicas, Universidad Nacional de La Plata, 1900 La Plata, Argentina
bAbteilung Kardiologie und Pneumologie, Univesität Göttingen, Göttingen, Germany

* Corresponding author. Tel.: +54-221-483-4833; fax: +54-221-425-5861. cicmes{at}infovia.com.ar

The stretch of the cardiac muscle is immediately followed by an increase in the contraction strength after which occurs a slow force increase (SFR) that takes several minutes to fully develop. The SFR was detected in a wide variety of experimental preparations including isolated myocytes, papillary muscles and/or trabeculae, left ventricle strips of failing human myocardium, in vitro isovolumic and in vivo volume-loaded hearts. It was established that the initial increase in force is due to an increase in myofilament Ca2+ responsiveness, whereas the SFR results from an increase in the Ca2+ transient. However, the mechanism(s) for this increase in the Ca2+ transient has remained undefined until the proposal of Na+/H+ exchanger (NHE) activation by stretch. Studies in multicellular cardiac muscle preparations from cat, rabbit, rat and failing human heart have shown evidence that the stretch induces a rise in intracellular Na+ ([Na+]i) through NHE activation, which subsequently leads to an increase in Ca2+ transient via reverse-mode Na+/Ca2+ (NCX) exchange. These experimental data agree with a theoretical ionic model of cardiomyocytes that predicted an increased Na+ influx and a concurrent increase in Ca2+ entry through NCX as the cause of the SFR to muscle stretch. However, there are aspects that await definitive demonstration, and perhaps subjected to species-related differences like the possibility of an autocrine/paracrine loop involving angiotensin II and endothelin as the underlying mechanism for stretch-induced NHE activation leading to the rise in [Na+]i and reverse-mode NCX.

KEYWORDS Angiotensin; Endothelins; Na/Ca-exchanger; Na/H-exchanger; Stretch/m-e coupling

1 Established investigators of Consejo Nacional de Investigaciones Científicas y Técnicas (Conicet) Argentina.


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