Growth hormone preserves cardiac sarcoplasmic reticulum Ca2+ release channels (ryanodine receptors) and enhances cardiac function in cardiomyopathic hamsters

doi:10.1016/S0008-6363(98)00095-9

Cardiovascular Research 1998 40(1):64-73; doi:10.1016/S0008-6363(98)00095-9
© 1998 by European Society of Cardiology

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Growth hormone preserves cardiac sarcoplasmic reticulum Ca²⁺ release channels (ryanodine receptors) and enhances cardiac function in cardiomyopathic hamsters

Takeshi Ueyama, Tomoko Ohkusa^*, Masafumi Yano and Masunori Matsuzaki

Second Department of Internal Medicine, Yamaguchi University School of Medicine, Ube, Yamaguchi 755, Japan

^* Corresponding author: Tel. 81-836-22-2248; Fax. 81-836-22-2246; e-mail: ohkusa@po.cc.yamaguchi-u.ac.jp

Objective: Growth hormone (GH) improves cardiac function inexperimental models of heart failure and human dilated cardiomyopathy.However, the mechanism by which GH increases myocardial contractilityis not entirely clear. Our aim was to examine the effects ofGH on cardiac function and cardiac sarcoplasmic reticulum Ca²⁺release channels (ryanodine receptors, RyR) in the hearts ofUM-X7.1 cardiomyopathic hamsters during the development of heartfailure. Methods: Experimental and healthy control hamsterswere examined at the age of 20 weeks. Recombinant human GH (2mg/kg/day, sc) or vehicle was then administered for 3 weeks.We examined (i) the in vivo left ventricular (LV) size and LVsystolic function using transthoracic echocardiography, (ii)the density (B_max) and affinity (K_d) of high-affinity [³H] ryanodinebinding sites in crude homogenates from normal and cardiomyopathichamster hearts. Results: Vehicle-treated UM-X7.1 hamsters exhibitedsignificant increases in left ventricular end-diastolic diameterand end-systolic diameter (LVESd), and a significant decreasein LV fractional shortening (FS). GH-treatment attenuated theincrease in LVESd and reduced the LV chamber size, and alsosignificantly increased LVFS. Vehicle-treated UM-X7.1 hamstersexhibited a significantly lower B_max than control hamsters (0.34±0.04vs 0.44±0.06 pmol/mg, p<0.05), and the treatment withGH in UM-X7.1 hamsters significantly attenuated the reductionof B_max {0.42±0.03 pmol/mg vs vehicle-treated group (0.34±0.04pmol/mg), p<0.05}. K_d did not differ significantly betweenthe experimental groups. In normal control hamsters, GH treatmentwith this dose did not significantly enhance LV systolic functionor the density of RyRs. There was no significant differencein terms of the connective-tissue volume- fraction, myocytesize and capillary density between the GH- and vehicle-treatedgroups of UM-X7.1 hamsters. Conclusions: GH treatment may improvecardiac function by preserving the density of RyRs and enhancingcellular function in cardiomyopathic hamster hearts.

KEYWORDS Cardiomyopathic hamster; Growth hormone; Heart failure; Ryanodine receptor; Sarcoplasmic reticulum

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