Localization of Functional Endothelin Receptor Signaling Complexes in Cardiac Transverse Tubules

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Abstract

Endothelin-1 (ET-1) is an autocrine factor in the mammalian heart important in enhancing cardiac performance, protecting against myocardial ischemia, and initiating the development of cardiac hypertrophy. The ET A receptor is a seven-transmembrane G-protein-coupled receptor whose precise subcellular localization in cardiac muscle is unknown. Here we used fluorescein ET-1 and 125I-ET-1 to provide evidence for ET-1 receptors in cardiac transverse tubules (T-tubules). Moreover, the ET A receptor and downstream effector phospholipase C-β 1, were co-localized within T-tubules using standard immunofluorescence techniques, and protein kinase C (PKC)-ε-enhanced green fluorescent protein bound reversibly to T-tubules upon activation. Localized photorelease of diacylglycerol further suggested compartmentation of PKC signaling, with release at the myocyte "surface" mimicking the negative inotropic effects of bath-applied PKC activators and "deep" release mimicking the positive inotropic effect of ET-1. The functional significance of T-tubular ET-1 receptors was further tested by rendering the T-tubule lumen inaccessible to bath-applied ET-1. Such "detubulated" cardiac myocytes showed no positive inotropic response to 20 nM ET-1, despite retaining both a nearly normal twitch response to field stimulation and a robust positive inotropic response to 20 nM isoproterenol. We propose that ET-1 enhances myocyte contractility by activating ETA receptor-phospholipase C-β1-PKC-ε signaling complexes preferentially localized in cardiac T-tubules. Compartmentation of ET-1 signaling complexes may explain the discordant effects of ET-1 versus bath applied PKC activators and may contribute to both the specificity and diversity of the cardiac actions of ET-1.

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Robu, V. G., Pfeiffer, E. S., Robia, S. L., Balijepalli, R. C., Pi, Y. Q., Kamp, T. J., & Walker, J. W. (2003). Localization of Functional Endothelin Receptor Signaling Complexes in Cardiac Transverse Tubules. Journal of Biological Chemistry, 278(48), 48154–48161. https://doi.org/10.1074/jbc.M304396200

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