Induction of Heme Oxygenase-1 Expression in Vascular Smooth Muscle Cells

Yet, Shaw‐Fang; Pellacani, Andrea; Patterson, Cam; Tan, Larissa; Folta, Sara C.; Foster, Lauren C.; Lee, Wen Sen; Hsieh, Chung Ming; Perrella, Mark A.

doi:10.1074/jbc.272.7.4295

Cited by 182 publications

(161 citation statements)

References 35 publications

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“…This include the ability of CO to promote vasodilatation (36) by the induction of smooth muscle cell relaxation (26,37). Vasodilatation may contribute to prevent vascular thrombosis, which would be important in suppressing graft rejection.…”

Section: Discussionmentioning

confidence: 99%

Carbon Monoxide Generated by Heme Oxygenase-1 Suppresses the Rejection of Mouse-to-Rat Cardiac Transplants

Sato

Balla

Otterbein

et al. 2001

The Journal of Immunology

440

338

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Mouse-to-rat cardiac transplants survive long term after transient complement depletion by cobra venom factor and T cell immunosuppression by cyclosporin A. Expression of heme oxygenase-1 (HO-1) by the graft vasculature is critical to achieve graft survival. In the present study, we asked whether this protective effect was attributable to the generation of one of the catabolic products of HO-1, carbon monoxide (CO). Our present data suggests that this is the case. Under the same immunosuppressive regimen that allows mouse-to-rat cardiac transplants to survive long term (i.e., cobra venom factor plus cyclosporin A), inhibition of HO-1 activity by tin protoporphyrin, caused graft rejection in 3–7 days. Rejection was associated with widespread platelet sequestration, thrombosis of coronary arterioles, myocardial infarction, and apoptosis of endothelial cells as well as cardiac myocytes. Under inhibition of HO-1 activity by tin protoporphyrin, exogenous CO suppressed graft rejection and restored long-term graft survival. This effect of CO was associated with inhibition of platelet aggregation, thrombosis, myocardial infarction, and apoptosis. We also found that expression of HO-1 by endothelial cells in vitro inhibits platelet aggregation and protects endothelial cells from apoptosis. Both these actions of HO-1 are mediated through the generation of CO. These data suggests that HO-1 suppresses the rejection of mouse-to-rat cardiac transplants through a mechanism that involves the generation of CO. Presumably CO suppresses graft rejection by inhibiting platelet aggregation that facilitates vascular thrombosis and myocardial infarction. Additional mechanisms by which CO overcomes graft rejection may involve its ability to suppress endothelial cell apoptosis.

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Section: Discussionmentioning

confidence: 99%

Carbon Monoxide Generated by Heme Oxygenase-1 Suppresses the Rejection of Mouse-to-Rat Cardiac Transplants

Sato

Balla

Otterbein

et al. 2001

The Journal of Immunology

440

338

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“…The similarities and diversities of the NO/NOS and CO/ HO systems were well established in numerous studies (11,14), but the interactions between these systems have not yet been elucidated. The interactive behavior of the two systems has been examined in monocytic cells (7), vascular endothelial cells (4), and vascular smooth muscle cells (22), and accumulating evidence from these studies has shown that the NO/NOS system induces the CO/HO system, while the CO/HO system reciprocally regulates the NO/NOS system. The relationship between the two systems in whole organs, on the other hand, has not been well studied, and it is unknown whether the two systems interact in the same manner in all organs or whether the two systems interact in an organ-specific manner.…”

Section: Real-time Reverse Transcriptase-polymerase Chain Reaction (Rmentioning

confidence: 99%

The reciprocal relationship between heme oxygenase and nitric oxide synthase in the organs of lipopolysaccharide-treated rodents

et al. 2009

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The production of nitric oxide (NO) by inducible NO synthase (NOS) and carbon monoxide (CO) by inducible heme oxygenase (HO) contributes greatly to endotoxemia. Reciprocal relationships have been proposed between the NO/NOS and CO/HO systems. However, the interaction between these systems during endotoxemia is unclear, and it is unknown whether the interactive behavior differs among organs. Using endotoxic rats, we studied the effects of the inducible NOS (iNOS) inhibitor L-canavanine (CAN), and the HO inhibitor zinc protoporphyrin (ZPP) on gene expression and protein levels of iNOS, endothelial NOS (eNOS), inducible HO (HO-1), and constitutive HO (HO-2) in the brain, lung, heart, liver and kidney tissue. Intravenous injection of LPS significantly increased iNOS and HO-1 gene expression in all organs. The effects of LPS on eNOS gene expression differed among organs, with increased expression in the liver and kidney, and no change in the lung, brain and heart. ZPP administration down-regulated the LPS-induced increase in HO-1 expression and produced a further increase in iNOS expression in all organs. These data suggest that the CO/HO system modifies the NO/NOS system in endotoxic organs, and that there were only minor organ-specific behaviors in terms of the relationship between these systems in the organs examined.Endotoxemia, which can lead to shock, is a detrimental consequence of severe Gram-negative bacterial infection. Endotoxic shock is initiated by the release of bacterial cell wall-derived lipopolysaccharide (LPS) and the subsequent production of cytokines and vasoactive mediators (13). Gaseous mediators, namely nitric oxide (NO) and carbon monoxide (CO), and the major endogenous sources of these mediators, nitric oxide synthase (NOS) and heme oxygenase (HO), serve a pivotal role in endotoxemia. NO is an extensively studied molecule, and is known for its vasorelaxation and oxidative stressor properties during endotoxemia and septic shock. NO is produced by three distinct NOS enzymes. Two of these NOS isozymes are predominantly constitutively expressed in endothelial cells (eNOS) and in neuronal cells (nNOS), whereas the expression of the third isozyme (iNOS) is inducible in a variety of cells (e.g., macrophages, hepatocytes, vascular smooth muscle cells and cardiac myocytes) by numerous stimuli, including LPS (5, 13). iNOS is responsible for producing most of the NO that causes hypotension and oxidative stress during endotoxic shock, while eNOS is reported to have only a minor role in the pathophysiology of endotoxemia (9, 18). CO has been perceived for many years to be a life-threatening gas; recently, however, CO has become recognized to have anti-inflammatory and vasorelaxative properties and is essential for life. HO is the rate-limiting enzyme in the catabolism of heme, a process that promotes the formation of equimolar amounts of the bile pigment biliverdin, free iron, and CO (1). Together with the anti-inflam-

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“…The common conception that these enzymes are merely components of a catabolic pathway that facilitates the elimination of toxic products from the organism has been disputed by strong evidence demonstrating that endogenously generated CO and bilirubin act as crucial effector molecules in the mitigation of vascular and cellular dysfunction (4 -12). Disparate conditions and a number of pathological states including hypoxia, endotoxic shock, atherosclerosis, and inflammation have been found to promote overexpression of the HO-1 gene and increased heme oxygenase activity (13)(14)(15)(16)(17)(18). Although the molecular mechanism(s) leading to HO-1 induction by these and other conditions remains to be fully elucidated, a common denominator that characterizes the prompt stimulation of HO-1 under most circumstances is the transient decrease in cellular glutathione levels and a drastic change in the redox status of the intracellular milieu (15, 19 -21).…”

mentioning

confidence: 99%

Induction of Heme Oxygenase 1 by Nitrosative Stress

Naughton

Foresti

Bains

et al. 2002

Journal of Biological Chemistry

106

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Heme oxygenase, the rate-limiting step in heme degradation to CO and bilirubin, exists in inducible (HO-1) 1 and constitutive (HO-2 and HO-3) isoforms, the synthesis and activities of which are differentially regulated in mammalian tissues (1-3). The common conception that these enzymes are merely components of a catabolic pathway that facilitates the elimination of toxic products from the organism has been disputed by strong evidence demonstrating that endogenously generated CO and bilirubin act as crucial effector molecules in the mitigation of vascular and cellular dysfunction (4 -12). Disparate conditions and a number of pathological states including hypoxia, endotoxic shock, atherosclerosis, and inflammation have been found to promote overexpression of the HO-1 gene and increased heme oxygenase activity (13-18). Although the molecular mechanism(s) leading to HO-1 induction by these and other conditions remains to be fully elucidated, a common denominator that characterizes the prompt stimulation of HO-1 under most circumstances is the transient decrease in cellular glutathione levels and a drastic change in the redox status of the intracellular milieu (15, 19 -21). It is not surprising, therefore, that conditions associated with increased production of reactive oxygen species and reactive nitrogen species (RNS) favor the activation of the HO-1/CO/bilirubin pathway, which is now regarded as an important cellular stratagem to counteract and resist different stress insults (3,22). In the context of redox reactions and signal transduction events that elicit the expression of HO-1 in vascular tissue, the gaseous molecule NO has recently been highlighted as an important biological modulator (see reviews in Refs. 22 and 23; Refs. 15 and 24). NO has been implicated in a wide range of processes critical to normal functions in the cardiovascular, nervous, and immune systems; the cytotoxic nature of NO has also been extensively emphasized when excessive production of this gas is triggered under certain pathological conditions (25). The conception that HO-1 might function to counteract the potential toxic effects evoked by NO first emerged from the discovery that certain NO-releasing agents can stimulate an increase in HO-1 transcript and heme oxygenase activity, resulting in protection against oxidative stress (26 -28). Subsequent reports have confirmed these findings (24, 29 -31), and more recent works have established that NO-related species (such as peroxynitrite and S-nitrosoglutathione) as well as endogenously generated NO and S-nitrosothiols are also capable of 32). In light of the rather complex and diverse chemistry of the NO group, which enables it to exist in a variety of interrelated redox-activated forms, investigations are now required to explore which additional NO * This work was supported by British Heart Foundation Grants PG/ 1999-005 and PG/2001-037 (to R. M.) and PG/2000 and by funds from the Dunhill Medical Trust. The National Heart Research Fund and the Wellcome Trust provided travel grants to p...

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Induction of Heme Oxygenase-1 Expression in Vascular Smooth Muscle Cells

Cited by 182 publications

References 35 publications

Carbon Monoxide Generated by Heme Oxygenase-1 Suppresses the Rejection of Mouse-to-Rat Cardiac Transplants

Carbon Monoxide Generated by Heme Oxygenase-1 Suppresses the Rejection of Mouse-to-Rat Cardiac Transplants

The reciprocal relationship between heme oxygenase and nitric oxide synthase in the organs of lipopolysaccharide-treated rodents

Induction of Heme Oxygenase 1 by Nitrosative Stress

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