Abstract

BackgroundVisfatin, a adipocytokine with insulin-mimetic effect, plays a role in endothelial angiogenesis. Hyperbaric oxygen (HBO) has been used in medical practice. However, the molecular mechanism of beneficial effects of HBO is poorly understood. We sought to investigate the cellular and molecular mechanisms of regulation of visfatin by HBO in human coronary arterial endothelial cells (CAECs).MethodsHuman CAECs were exposed to 2.5 atmosphere absolute (ATA) of oxygen in a hyperbaric chamber. Western blot, real-time polymerase chain reaction, and promoter activity assay were performed. In vitro glucose uptake and tube formation was detected.ResultsVisfatin protein (2.55-fold) and mRNA (2.53-fold) expression were significantly increased after exposure to 2.5 ATA HBO for 4 to 6 h. Addition of SP600125 and JNK siRNA 30 min before HBO inhibited the induction of visfatin protein. HBO also significantly increased DNA-protein binding activity of AP-1 and visfatin promoter activity. Addition of SP600125 and TNF-α monoclonal antibody 30 min before HBO abolished the DNA-protein binding activity and visfatin promoter activity induced by HBO. HBO significantly increased secretion of TNF-α from cultured human CAECs. Exogenous addition of TNF-α significantly increased visfatin protein expression while TNF-α antibody and TNF-α receptor antibody blocked the induction of visfatin protein expression induced by HBO. HBO increased glucose uptake in human CAECs as HBO and visfatin siRNA and TNF-α antibody attenuated the glucose uptake induced by HBO. HBO significantly increased the tube formation of human CAECs while visfatin siRNA, TNF-α antibody inhibited the tube formation induced by HBO.ConclusionsHBO activates visfatin expression in cultured human CAECs. HBO-induced visfatin is mediated by TNF-α and at least in part through JNK pathway.

Highlights

  • Visfatin, a adipocytokine with insulin-mimetic effect, plays a role in endothelial angiogenesis

  • Visfatin protein level still maintained elevated after 8 h of Hyperbaric oxygen (HBO) treatment, the level of visfatin protein tended to return to baseline level

  • Because visfatin protein was maximally induced at 6 h after HBO treatment, the following experiments were set for HBO treatment for 6 hours

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Summary

Introduction

A adipocytokine with insulin-mimetic effect, plays a role in endothelial angiogenesis. The molecular mechanism of beneficial effects of HBO is poorly understood. We sought to investigate the cellular and molecular mechanisms of regulation of visfatin by HBO in human coronary arterial endothelial cells (CAECs). Hyperbaric oxygen (HBO) therapy provides a significant increase in oxygen content in the hypoperfused tissue and the elevation in oxygen content in the hypoxic tissue induces powerful positive changes in ischemic repair process [13]. HBO therapy promotes wound healing by directly enhancing fibroblastic replication, collagen synthesis, and the process of neovascularization in ischemic tissue [15]

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