| Literature DB >> 26392029 |
Anita Ongherth1, Sebastian Pasch1, Christina M Wuertz1, Karolin Nowak2, Naim Kittana1, Cleo A Weis3, Aline Jatho1, Christiane Vettel4, Malte Tiburcy1, Karl Toischer5, Gerd Hasenfuss5, Wolfram-Hubertus Zimmermann1, Thomas Wieland6, Susanne Lutz7.
Abstract
Cardiac remodeling, a hallmark of heart disease, is associated with intense auto- and paracrine signaling leading to cardiac fibrosis. We hypothesized that the specific mediator of Gq/11-dependent RhoA activation p63RhoGEF, which is expressed in cardiac fibroblasts, plays a role in the underlying processes. We could show that p63RhoGEF is up-regulated in mouse hearts subjected to transverse aortic constriction (TAC). In an engineered heart muscle model (EHM), p63RhoGEF expression in cardiac fibroblasts increased resting and twitch tensions, and the dominant negative p63ΔN decreased both. In an engineered connective tissue model (ECT), p63RhoGEF increased tissue stiffness and its knockdown as well as p63ΔN reduced stiffness. In 2D cultures of neonatal rat cardiac fibroblasts, p63RhoGEF regulated the angiotensin II (Ang II)-dependent RhoA activation, the activation of the serum response factor, and the expression and secretion of the connective tissue growth factor (CTGF). All these processes were inhibited by the knockdown of p63RhoGEF or by p63ΔN likely based on their negative influence on the actin cytoskeleton. Moreover, we show that p63RhoGEF also regulates CTGF in engineered tissues and correlates with it in the TAC model. Finally, confocal studies revealed a closely related localization of p63RhoGEF and CTGF in the trans-Golgi network.Entities:
Keywords: Cardiac remodeling; Connective tissue growth factor; RhoA; p63RhoGEF
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Year: 2015 PMID: 26392029 DOI: 10.1016/j.yjmcc.2015.09.009
Source DB: PubMed Journal: J Mol Cell Cardiol ISSN: 0022-2828 Impact factor: 5.000