Adenylyl Cyclase Subtype–Specific Compartmentalization

Author:

Timofeyev Valeriy1,Myers Richard E.1,Kim Hyo Jeong1,Woltz Ryan L.1,Sirish Padmini1,Heiserman James P.1,Li Ning1,Singapuri Anil1,Tang Tong1,Yarov-Yarovoy Vladimir1,Yamoah Ebenezer N.1,Hammond H. Kirk1,Chiamvimonvat Nipavan1

Affiliation:

1. From the Division of Cardiovascular Medicine (V.T., R.E.M., R.L.W., P.S., J.P.H., N.L., A.S., N.C.), Center for Neuroscience (H.J.K., E.N.Y.), and Department of Physiology and Membrane Biology (V.Y.-Y.), University of California, Davis; Department of Medicine, University of California, San Diego (T.T., H.K.H.); Department of Veterans Affairs, San Diego Healthcare System, San Diego, CA (H.K.H.); and Department of Veterans Affairs, Northern California Health Care System, Mather (N.C.).

Abstract

Rationale: Adenylyl cyclase (AC) represents one of the principal molecules in the β-adrenergic receptor signaling pathway, responsible for the conversion of ATP to the second messenger, cAMP. AC types 5 (AC V ) and 6 (AC VI ) are the 2 main isoforms in the heart. Although highly homologous in sequence, these 2 proteins play different roles during the development of heart failure. Caveolin-3 is a scaffolding protein, integrating many intracellular signaling molecules in specialized areas called caveolae. In cardiomyocytes, caveolin is located predominantly along invaginations of the cell membrane known as t-tubules. Objective: We take advantage of AC V and AC VI knockout mouse models to test the hypothesis that there is distinct compartmentalization of these isoforms in ventricular myocytes. Methods and Results: We demonstrate that AC V and AC VI isoforms exhibit distinct subcellular localization. The AC VI isoform is localized in the plasma membrane outside the t-tubular region and is responsible for β 1 -adrenergic receptor signaling–mediated enhancement of the L-type Ca 2+ current ( I Ca,L ) in ventricular myocytes. In contrast, the AC V isoform is localized mainly in the t-tubular region where its influence on I Ca,L is restricted by phosphodiesterase. We further demonstrate that the interaction between caveolin-3 with AC V and phosphodiesterase is responsible for the compartmentalization of AC V signaling. Conclusions: Our results provide new insights into the compartmentalization of the 2 AC isoforms in the regulation of I Ca,L in ventricular myocytes. Because caveolae are found in most mammalian cells, the mechanism of β- adrenergic receptor and AC compartmentalization may also be important for β-adrenergic receptor signaling in other cell types.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine,Physiology

Reference39 articles.

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