AKT-independent activation of p38 MAP kinase promotes vascular calcification

AKT-independent activation of p38 MAP kinase promotes vascular calcification

Vascular calcification is prevalent in patients with atherosclerosis, and oxidative stress promotes pathogenesis of atherosclerosis. We have previously reported that activation of AKT by oxidative stress induces vascular calcification. Using sodium dichloroacetate (DCA), a previously reported small...

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Main Authors: Youfeng Yang, Yong Sun, Jianye Chen, Wayne E. Bradley, Louis J. Dell’Italia, Hui Wu, Yabing Chen
Format: Article
Language:English
Published: Elsevier 2018-06-01
Series:Redox Biology
Online Access:http://www.sciencedirect.com/science/article/pii/S2213231717309801
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spelling doaj-b071f2bd138a47c08a7c183c0993f2b52020-11-25T01:49:52ZengElsevierRedox Biology2213-23172018-06-011697103AKT-independent activation of p38 MAP kinase promotes vascular calcificationYoufeng Yang0Yong Sun1Jianye Chen2Wayne E. Bradley3Louis J. Dell’Italia4Hui Wu5Yabing Chen6Department of Pathology, University of Alabama at Birmingham, 1825 University Blvd, 614 Shelby Biomedical Research Building, Birmingham, AL 35294, USADepartment of Pathology, University of Alabama at Birmingham, 1825 University Blvd, 614 Shelby Biomedical Research Building, Birmingham, AL 35294, USADepartment of Pathology, University of Alabama at Birmingham, 1825 University Blvd, 614 Shelby Biomedical Research Building, Birmingham, AL 35294, USADepartment of Medicine, University of Alabama at Birmingham, USADepartment of Medicine, University of Alabama at Birmingham, USADepartment of Pediatric Dentistry, University of Alabama at Birmingham, USADepartment of Pathology, University of Alabama at Birmingham, 1825 University Blvd, 614 Shelby Biomedical Research Building, Birmingham, AL 35294, USA; Research Department, Veterans Affairs Birmingham Medical Center, Birmingham, AL, USA; Corresponding author.Vascular calcification is prevalent in patients with atherosclerosis, and oxidative stress promotes pathogenesis of atherosclerosis. We have previously reported that activation of AKT by oxidative stress induces vascular calcification. Using sodium dichloroacetate (DCA), a previously reported small molecule inhibitor of AKT, the present studies uncovered an AKT-independent mechanism in regulating vascular calcification.We found that DCA dose-dependently induced calcification of vascular smooth muscle cells (VSMC) in vitro and aortic rings ex vivo. Furthermore, DCA markedly enhanced vascular calcification in atherosclerotic ApoE knockout mice in vivo. DCA-induced VSMC calcification was associated with increased Runx2, but not via activation of AKT, a key upstream signal that upregulates Runx2 during VSMC calcification. In contrast, DCA inhibited AKT activation and induced activation of p38 MAPK in calcified atherosclerotic lesions in vivo and calcified VSMC in vitro. Using a pharmacological inhibitor and shRNA for p38 MAPK, we demonstrated that inhibition of p38 MAPK blocked DCA-induced Runx2 upregulation and VSMC calcification. Furthermore, Runx2 deletion attenuated DCA-induced VSMC calcification. Immunoprecipitation analysis revealed association of p38 MAPK with Runx2, which was enhanced by DCA treatment. Knockdown p38 MAPK inhibited DCA-induced Runx2 transactivity, supporting the function of p38 MAPK in regulating Runx2 transactivity.Our studies have uncovered a new function of DCA in regulating vascular calcification, via AKT-independent activation of p38 MAPK. Furthermore, we have identified novel interaction between p38 MAPK and Runx2 enhances Runx2 transactivity, thus promoting VSMC calcification. These results revealed a novel signaling mechanism underlying DCA-induced vascular calcification, and offer opportunities to identify new therapeutic targets. Keywords: Oxidative stress, Vascular calcification, P38 MAPK, AKT, Runx2http://www.sciencedirect.com/science/article/pii/S2213231717309801
collection DOAJ
language English
format Article
sources DOAJ
author Youfeng Yang
Yong Sun
Jianye Chen
Wayne E. Bradley
Louis J. Dell’Italia
Hui Wu
Yabing Chen
spellingShingle Youfeng Yang
Yong Sun
Jianye Chen
Wayne E. Bradley
Louis J. Dell’Italia
Hui Wu
Yabing Chen
AKT-independent activation of p38 MAP kinase promotes vascular calcification
Redox Biology
author_facet Youfeng Yang
Yong Sun
Jianye Chen
Wayne E. Bradley
Louis J. Dell’Italia
Hui Wu
Yabing Chen
author_sort Youfeng Yang
title AKT-independent activation of p38 MAP kinase promotes vascular calcification
title_short AKT-independent activation of p38 MAP kinase promotes vascular calcification
title_full AKT-independent activation of p38 MAP kinase promotes vascular calcification
title_fullStr AKT-independent activation of p38 MAP kinase promotes vascular calcification
title_full_unstemmed AKT-independent activation of p38 MAP kinase promotes vascular calcification
title_sort akt-independent activation of p38 map kinase promotes vascular calcification
publisher Elsevier
series Redox Biology
issn 2213-2317
publishDate 2018-06-01
description Vascular calcification is prevalent in patients with atherosclerosis, and oxidative stress promotes pathogenesis of atherosclerosis. We have previously reported that activation of AKT by oxidative stress induces vascular calcification. Using sodium dichloroacetate (DCA), a previously reported small molecule inhibitor of AKT, the present studies uncovered an AKT-independent mechanism in regulating vascular calcification.We found that DCA dose-dependently induced calcification of vascular smooth muscle cells (VSMC) in vitro and aortic rings ex vivo. Furthermore, DCA markedly enhanced vascular calcification in atherosclerotic ApoE knockout mice in vivo. DCA-induced VSMC calcification was associated with increased Runx2, but not via activation of AKT, a key upstream signal that upregulates Runx2 during VSMC calcification. In contrast, DCA inhibited AKT activation and induced activation of p38 MAPK in calcified atherosclerotic lesions in vivo and calcified VSMC in vitro. Using a pharmacological inhibitor and shRNA for p38 MAPK, we demonstrated that inhibition of p38 MAPK blocked DCA-induced Runx2 upregulation and VSMC calcification. Furthermore, Runx2 deletion attenuated DCA-induced VSMC calcification. Immunoprecipitation analysis revealed association of p38 MAPK with Runx2, which was enhanced by DCA treatment. Knockdown p38 MAPK inhibited DCA-induced Runx2 transactivity, supporting the function of p38 MAPK in regulating Runx2 transactivity.Our studies have uncovered a new function of DCA in regulating vascular calcification, via AKT-independent activation of p38 MAPK. Furthermore, we have identified novel interaction between p38 MAPK and Runx2 enhances Runx2 transactivity, thus promoting VSMC calcification. These results revealed a novel signaling mechanism underlying DCA-induced vascular calcification, and offer opportunities to identify new therapeutic targets. Keywords: Oxidative stress, Vascular calcification, P38 MAPK, AKT, Runx2
url http://www.sciencedirect.com/science/article/pii/S2213231717309801
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