Volume 52, Issue 2 , Pages 493-501, February 2012
Focal adhesion kinase governs cardiac concentric hypertrophic growth by activating the AKT and mTOR pathways
Abstract
The heart responds to sustained overload by hypertrophic growth in which the myocytes distinctly thicken or elongate on increases in systolic or diastolic stress. Though potentially adaptive, hypertrophy itself may predispose to cardiac dysfunction in pathological settings. The mechanisms underlying the diverse morphology and outcomes of hypertrophy are uncertain. Here we used a focal adhesion kinase (FAK) cardiac-specific transgenic mice model (FAK-Tg) to explore the function of this non-receptor tyrosine kinase on the regulation of myocyte growth. FAK-Tg mice displayed a phenocopy of concentric cardiac hypertrophy, reflecting the relative thickening of the individual myocytes. Moreover, FAK-Tg mice showed structural, functional and molecular features of a compensated hypertrophic growth, and preserved responses to chronic pressure overload. Mechanistically, FAK overexpression resulted in enhanced myocardial FAK activity, which was proven by treatment with a selective FAK inhibitor to be required for the cardiac hypertrophy in this model. Our results indicate that upregulation of FAK does not affect the activity of Src/ERK1/2 pathway, but stimulated signaling by a cascade that encompasses PI3K, AKT, mTOR, S6K and rpS6. Moreover, inhibition of the mTOR complex by rapamycin extinguished the cardiac hypertrophy of the transgenic FAK mice. These findings uncover a unique role for FAK in regulating the signaling mechanisms that governs the selective myocyte growth in width, likely controlling the activity of PI3K/AKT/mTOR pathway, and suggest that FAK activation could be important for the adaptive response to increases in cardiac afterload. This article is part of a Special Issue entitled “Local Signaling in Myocytes”.
► Hypertrophy can be adaptive or pathological. ► Cardiac myocyte-FAK overexpression in mice induced compensated cardiac hypertrophy. ► Upregulation of FAK was accompanied by activation of PI3K, AKT, mTOR, S6K and rpS6. ► Inhibition of the mTOR complex by rapamycin extinguished the cardiac hypertrophy. ► FAK activation may be important for the adaptive responses to increases in cardiac afterload.
Abbreviations: FAK, focal adhesion kinase, FAK-Tg, cardiac-specific FAK transgenic mice model, FAKi, pharmacological FAK inhibitor (PF 573228), RP, rapamycin, TAC, thoracic aortic constriction
Keywords: Cardiac myocytes, Cardiac failure, Mechanotransduction, Signal transduction, Transgenic mice
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PII: S0022-2828(11)00442-1
doi:10.1016/j.yjmcc.2011.10.015
© 2011 Elsevier Ltd. All rights reserved.
Volume 52, Issue 2 , Pages 493-501, February 2012
