FoxO4 Promotes Early Inflammatory Response Upon Myocardial Infarction via Endothelial Arg1. Issue 11 (6th November 2015)
- Record Type:
- Journal Article
- Title:
- FoxO4 Promotes Early Inflammatory Response Upon Myocardial Infarction via Endothelial Arg1. Issue 11 (6th November 2015)
- Main Title:
- FoxO4 Promotes Early Inflammatory Response Upon Myocardial Infarction via Endothelial Arg1
- Authors:
- Zhu, Min
Goetsch, Sean C.
Wang, Zhaoning
Luo, Robert
Hill, Joseph A.
Schneider, Jay
Morris, Sidney M.
Liu, Zhi-Ping - Abstract:
- Abstract : Rationale: : Inflammation in post–myocardial infarction (MI) is necessary for myocyte repair and wound healing. Unfortunately, it is also a key component of subsequent heart failure pathology. Transcription factor forkhead box O4 (FoxO4) regulates a variety of biological processes, including inflammation. However, its role in MI remains unknown. Objective: : To test the hypothesis that FoxO4 promotes early post-MI inflammation via endothelial arginase 1 (Arg1). Methods and Results: : We induced MI in wild-type and FoxO4 −/− mice. FoxO4 −/− mice had a significantly higher post-MI survival, better cardiac function, and reduced infarct size. FoxO4 −/− hearts had significantly fewer neutrophils, reduced expression of cytokines, and competitive nitric oxide synthase inhibitor Arg1. We generated conditional FoxO4 knockout mice with FoxO4 deleted in cardiac mycoytes or endothelial cells. FoxO4 endothelial cell–specific knockout mice showed significant post-MI improvement of cardiac function and reduction of neutrophil accumulation and cytokine expression, whereas FoxO4 cardiac mycoyte–specific knockout mice had no significant difference in cardiac function and post-MI inflammation from those of control littermates. FoxO4 binds the Foxo-binding site in the Arg1 promoter and activates Arg1 transcription. FoxO4 knockdown in human aortic endothelial cells upregulated nitric oxide on ischemia and suppressed monocyte adhesion that can be reversed by ectopic-expression of Arg1.Abstract : Rationale: : Inflammation in post–myocardial infarction (MI) is necessary for myocyte repair and wound healing. Unfortunately, it is also a key component of subsequent heart failure pathology. Transcription factor forkhead box O4 (FoxO4) regulates a variety of biological processes, including inflammation. However, its role in MI remains unknown. Objective: : To test the hypothesis that FoxO4 promotes early post-MI inflammation via endothelial arginase 1 (Arg1). Methods and Results: : We induced MI in wild-type and FoxO4 −/− mice. FoxO4 −/− mice had a significantly higher post-MI survival, better cardiac function, and reduced infarct size. FoxO4 −/− hearts had significantly fewer neutrophils, reduced expression of cytokines, and competitive nitric oxide synthase inhibitor Arg1. We generated conditional FoxO4 knockout mice with FoxO4 deleted in cardiac mycoytes or endothelial cells. FoxO4 endothelial cell–specific knockout mice showed significant post-MI improvement of cardiac function and reduction of neutrophil accumulation and cytokine expression, whereas FoxO4 cardiac mycoyte–specific knockout mice had no significant difference in cardiac function and post-MI inflammation from those of control littermates. FoxO4 binds the Foxo-binding site in the Arg1 promoter and activates Arg1 transcription. FoxO4 knockdown in human aortic endothelial cells upregulated nitric oxide on ischemia and suppressed monocyte adhesion that can be reversed by ectopic-expression of Arg1. Furthermore, chemical inhibition of Arg1 in wild-type mice had similar cardioprotection and reduced inflammation after MI as FoxO4 inactivation and administration of nitric oxide synthase inhibitor to FoxO4 KO mice reversed the beneficial effects of FoxO4 deletion on post-MI cardiac function. Conclusions: : FoxO4 activates Arg1 transcription in endothelial cells in response to MI, leading to downregulation of nitric oxide and upregulation of neutrophil infiltration to the infarct area. Abstract : Supplemental Digital Content is available in the text. … (more)
- Is Part Of:
- Circulation research. Volume 117:Issue 11(2015)
- Journal:
- Circulation research
- Issue:
- Volume 117:Issue 11(2015)
- Issue Display:
- Volume 117, Issue 11 (2015)
- Year:
- 2015
- Volume:
- 117
- Issue:
- 11
- Issue Sort Value:
- 2015-0117-0011-0000
- Page Start:
- Page End:
- Publication Date:
- 2015-11-06
- Subjects:
- arginase -- endothelial cells -- FoxO4 protein, mouse -- inflammation -- myocardial infarction
Cardiovascular system -- Periodicals
Blood -- Circulation -- Periodicals
Blood Circulation
Cardiovascular System
Vascular Diseases
Sang -- Circulation -- Périodiques
Appareil cardiovasculaire -- Périodiques
612.1 - Journal URLs:
- http://circres.ahajournals.org/ ↗
http://www.circresaha.org ↗
http://journals.lww.com ↗ - DOI:
- 10.1161/CIRCRESAHA.115.306919 ↗
- Languages:
- English
- ISSNs:
- 0009-7330
- Deposit Type:
- Legaldeposit
- View Content:
- Available online (eLD content is only available in our Reading Rooms) ↗
- Physical Locations:
- British Library DSC - 3265.300000
British Library DSC - BLDSS-3PM
British Library STI - ELD Digital store - Ingest File:
- 5143.xml