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  2. Arginase-II induces vascular smooth muscle cell senescence and apoptosis through p66Shc and p53 independently of its l-arginine ureahydrolase activity: implications for atherosclerotic plaque vulnerability

Arginase-II induces vascular smooth muscle cell senescence and apoptosis through p66Shc and p53 independently of its l-arginine ureahydrolase activity: implications for atherosclerotic plaque vulnerability

  • J Am Heart Assoc. 2013 Jul 5;2(4):e000096. doi: 10.1161/JAHA.113.000096.
Yuyan Xiong 1 Yi Yu Jean-Pierre Montani Zhihong Yang Xiu-Fen Ming
Affiliations

Affiliation

  • 1 Vascular Biology, Department of Medicine, Division of Physiology, Faculty of Science, University of Fribourg, Chemin du Musée 5, Fribourg, CH-1700, Switzerland.
Abstract

Background: Vascular smooth muscle cell (VSMC) senescence and Apoptosis are involved in atherosclerotic plaque vulnerability. Arginase-II (Arg-II) has been shown to promote vascular dysfunction and plaque vulnerability phenotypes in mice through uncoupling of endothelial nitric oxide synthase and activation of macrophage inflammation. The function of Arg-II in VSMCs with respect to plaque vulnerability is unknown. This study investigated the functions of Arg-II in VSMCs linking to plaque vulnerability.

Methods and results: In vitro studies were performed on VSMCs isolated from human umbilical veins, whereas in vivo studies were performed on atherosclerosis-prone Apolipoprotein E-deficient (apoE(-/-)) mice. In nonsenescent VSMCs, overexpressing wild-type Arg-II or an l-arginine ureahydrolase inactive Arg-II mutant (H160F) caused similar effects on mitochondrial dysfunction, cell Apoptosis, and senescence, which were abrogated by silencing p66Shc or p53. The activation of p66Shc but not p53 by Arg-II was dependent on extracellular signal-regulated kinases (ERKs) and sequential activation of 40S ribosomal protein S6 kinase 1 (S6K1)-c-Jun N-terminal kinases (JNKs). In senescent VSMCs, Arg-II and S6K1, ERK-p66Shc, and p53 signaling levels were increased. Silencing Arg-II reduced all these signalings and cell senescence/Apoptosis. Conversely, silencing p66Shc reduced ERK and S6K1 signaling and Arg-II levels and cell senescence/Apoptosis. Furthermore, genetic ablation of Arg-II in apoE(-/-) mice reduced the aforementioned signaling and apoptotic VSMCs in the plaque of aortic roots.

Conclusions: Arg-II, independently of its l-arginine ureahydrolase activity, promotes mitochondrial dysfunction leading to VSMC senescence/Apoptosis through complex positive crosstalk among S6K1-JNK, ERK, p66Shc, and p53, contributing to atherosclerotic vulnerability phenotypes in mice.

Keywords

apoptosis; arginase; p53; p66Shc; vascular smooth muscle cells.

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