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Research Article Free access | 10.1172/JCI118346

Alteration of growth responses in established cardiac pressure overload hypertrophy in rats with aortic banding.

H Schunkert, E O Weinberg, G Bruckschlegel, A J Riegger, and B H Lorell

The Charles A. Dana Research Institute and Harvard-Thorndike Laboratory, Beth Israel Hospital, Boston, Massachusetts 02215, USA.

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The Charles A. Dana Research Institute and Harvard-Thorndike Laboratory, Beth Israel Hospital, Boston, Massachusetts 02215, USA.

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The Charles A. Dana Research Institute and Harvard-Thorndike Laboratory, Beth Israel Hospital, Boston, Massachusetts 02215, USA.

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The Charles A. Dana Research Institute and Harvard-Thorndike Laboratory, Beth Israel Hospital, Boston, Massachusetts 02215, USA.

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The Charles A. Dana Research Institute and Harvard-Thorndike Laboratory, Beth Israel Hospital, Boston, Massachusetts 02215, USA.

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Published December 1, 1995 - More info

Published in Volume 96, Issue 6 on December 1, 1995
J Clin Invest. 1995;96(6):2768–2774. https://doi.org/10.1172/JCI118346.
© 1995 The American Society for Clinical Investigation
Published December 1, 1995 - Version history
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Abstract

We examined the acute effects of elevated wall stress, norepinephrine, and angiotensin II on cardiac protein synthesis as well as protooncogene expression in hearts with established pressure overload left ventricular hypertrophy. Isolated rat hearts with chronic hypertrophy (LVH) were studied 12 wk after ascending aortic banding when systolic function was fully maintained. New protein synthesis (incorporation of [3H]phenylalanine [Phe]) was analyzed in isolated perfused rat hearts after a 3-h protocol; c-fos, c-jun, c-myc, and early growth response gene-1 (EGR-1) mRNA levels (Northern blot) were studied over a time course from 15 to 240 min of perfusion. Under baseline conditions (i.e., before mechanical or neurohormonal stimulation), [3H]-Phe-incorporation (280 nmoles/gram protein/h) and protooncogene mRNA levels were similar in age-matched control and LVH hearts. However, hearts with chronic LVH were characterized by a markedly blunted or absent [3H]-Phe-incorporation after acute imposition of isovolumic systolic load (90 mmHg/gram left ventricle), as well as norepinephrine (10(-6)M), or angiotensin II infusion (10(-8)M plus prazosin 10(-7)M) compared with nonhypertrophied control hearts. Similarly, stimulation of LVH hearts with acute systolic load or norepinephrine was associated with a significantly blunted increase of protooncogene mRNA levels relative to control hearts. The blunted induction of c-fos mRNA in LVH hearts was not due to feedback inhibition, since cycloheximide perfusion of hearts exposed to elevated wall stress further increased the differences between age-matched control and LVH hearts. The data suggest that acute molecular growth responses to mechanical or neurohormonal stimulation are altered in rat hearts with established LVH relative to nonhypertrophied control hearts. This alteration of molecular adaptations in hearts with compensatory hypertrophy may prevent inappropriate excess cardiac growth in response to mechanical and neurohormonal stimuli.

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