Nitric oxide: orchestrating hypoxia regulation through mitochondrial respiration and the endoplasmic reticulum stress response

Xu, Weiming; Charles, Ian G.; Moncada, Salvador

doi:10.1038/sj.cr.7290267

Cited by 78 publications

(52 citation statements)

References 16 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Hypoxia is known to upregulate transcription factor HIF1 activating expression of genes involved in angiogenesis [43]. However, it was demonstrated that co-existence of both hypoxia and lower NO concentration caused a rapid decrease in HIF1 [44,45] that may represent one of the mechanisms involved in anti-angiogenic efect of NO.…”

Section: Discussionmentioning

confidence: 99%

Ultrastructure and histochemistry of rat myocardial capillary endothelial cells in response to diabetes and hypertension

et al. 2005

View full text Add to dashboard Cite

Insufficient growth and rarefaction of capillaries, followed by endothelial dysfunction may represent one of the most critical mechanisms involved in heart damage. In this study we examined histochemical and ultrastructural changes in myocardial capillary endothelium in two models of heart failure streptozotocin-induced diabetes mellitus (STZ) and NOdeficient hypertension in male Wistar rats. Diabetes was induced by a single i.v. dose of STZ (45 mg/kg) and chronic 9-week stage was analysed. To induce NO-deficient hypertension, animals were treated with inhibitor of NO synthase Lnitroarginine methylester (L-NAME) (40 mg/kg) for 4 weeks. Left ventricular tissue was processed for enzyme catalytic histochemistry of capillary alkaline phosphatase (AlPh), dipeptidyl peptidase IV (DPP IV), and endothelial NO synthase/NADPH-diaphorase (NOS) and for ultrastructural analysis. In diabetic and hypertensive rats, lower/absent AlPh and DPP IV activities were found in focal micro-areas. NOS activity was significantly reduced and persisted only locally. Quantitative evaluation demonstrated reduction of reaction product intensity of AlPh, DPP and NOS by 49.50%, 74.36%, 20.05% in diabetic and 62.93%, 82.71%, 37.65% in hypertensive rats. Subcellular alterations of endothelial cells were found in heart of both groups suggesting injury of capillary function as well as compensatory processes. Endothelial injury was more significant in diabetic animals, in contrast the adaptation was more evident in hypertensive ones. Concluding: both STZ-induced diabetes-and NO-deficient hypertension-related cardiomyopathy were accompanied by similar features of structural remodelling of cardiac capillary network manifested as angiogenesis and angiopathy. The latter was however, predominant and may accelerate disappearance of capillary endothelium contributing to myocardial dysfunction.

show abstract

Section: Discussionmentioning

confidence: 99%

Ultrastructure and histochemistry of rat myocardial capillary endothelial cells in response to diabetes and hypertension

et al. 2005

View full text Add to dashboard Cite

show abstract

“…Thus, it has been documented that NO exerts several actions on cell respiration, particularly that NO is able to inhibit complex IV in the respiratory chain on mitochondria (Brunori et al, 2004). As a result of this inhibition, NO has been reported to posses both pro-apoptotic and anti-apoptotic effects (Beltran et al, 2000;Xu et al, 2005). Because apoptosis appears to be the main mechanism leading to oligodendrocyte death in this model (Arnett et al, 2002), it is possible that differences in time, dose, and site of NO secretion by the different NOS isoforms in response to cuprizone may lead to divergent effects in oligodendrocyte apoptosis and, therefore, explain the differences between the various NOS mutant strains and wild-type mice.…”

Section: Discussionmentioning

confidence: 99%

Neuronal Nitric Oxide Synthase Plays a Key Role in CNS Demyelination

Liñares¹,

Taconis²,

Mañá³

et al. 2006

J. Neurosci.

View full text Add to dashboard Cite

Nitric oxide (NO) is a small, short-lived molecule released from a variety of cells that is implicated in a multitude of biological processes.In pathological conditions, overproduction of NO may lead to the generation of highly reactive species, such as peroxynitrite and stable nitrosothiols, that may cause irreversible cell damage. Accordingly, several studies have suggested that NO may be involved in the pathogenesis of various neuroinflammatory/degenerative diseases. Increased concentrations of NO in the CNS in such cases are usually attributed to an increase in the inducible isoform of NO synthase (iNOS) usually produced by inflammatory cells. However, recent reports have suggested that the constitutive isoforms of NOS, neuronal (nNOS) and endothelial (eNOS), can also play a role. Here we examined the role that the constitutive isoforms of NOS might play in the cuprizone-induced model of demyelination/remyelination. Our results demonstrate that demyelination was greatly prevented in mice lacking nNOS. Protection was associated with a dramatic increase in mature oligodendrocyte survival and a decrease in apoptosis. Moreover, nNOS Ϫ/Ϫ mice did not respond to cuprizone with the extensive recruitment of microglia/macrophages and astrocytes, which is a typical feature in wild-type mice. Although demyelinating less, nNOS Ϫ/Ϫ mice exhibited a delay in remyelination. In eNOS Ϫ/Ϫ mice, demyelination progressed to the same extent as in wild type, but they showed a slight delay in spontaneous remyelination. In conclusion, this study highlights the importance of considering the source of NO when assessing its role in neuroinflammation/degeneration and emphasizes the differing pathological effects driven by the different NOS isoforms.

show abstract

“…The very high levels of NO shown in the present study are capable of inhibiting oxygen consumption by the mitochondria sufficient to decrease ATP synthesis. This can create a condition we have called 'nitroxia', which is associated with high levels of NO, oxygen and impaired mitochondrial bioenergetics [5,6]. The highly reducing status of the mitochondrial respiratory chain in the presence of oxygen will then promote superoxide formation.…”

mentioning

confidence: 99%

mentioning

confidence: 99%

“…However, the story became more complex with the recognition that NO serves as a ligand for other haem proteins such as COX (cytochrome c oxidase) in the mitochondria and haemoglobin in the red blood cell [2,3]. The fact that NO interacts with the haem groups that normally bind oxygen essentially expanded the role of NO in cell signalling from a simple haem ligand to a regulatory modulator of oxygen-sensitive processes [4][5][6].Since both COX and sGC frequently co-exist within the same cell, the relative sensitivity of the two pathways to NO should determine the ultimate biological effect. It has been shown that activation of sGC occurs at much lower concentrations of NO than inhibition of COX, but these studies have not addressed the sensitivity of these pathways using endogenous NO formation; nor have they investigated the influence of oxygen on this relative sensitivity in a cellular setting [7].…”

mentioning

confidence: 99%

See 1 more Smart Citation

Evidence for oxygen as the master regulator of the responsiveness of soluble guanylate cyclase and cytochrome c oxidase to nitric oxide

Landar

Darley‐Usmar

2007

Biochemical Journal

View full text Add to dashboard Cite

Haem is used as a versatile receptor for redox active molecules; most notably NO (nitric oxide) and oxygen. Three haemcontaining proteins, myoglobin, haemoglobin and cytochrome c oxidase, are now known to bind NO, and in all these cases competition with oxygen plays an important role in the biological outcome. NO also binds to the haem group of sGC (soluble guanylate cyclase) and initiates signal transduction through the formation of cGMP in a process that is oxygen-independent. From biochemical studies, it has been shown that sGC is substantially more sensitive to NO than is cytochrome c oxidase, but a direct comparison in a cellular setting under various oxygen levels has not been reported previously. In this issue of the Biochemical Journal, Cadenas and co-workers reveal how oxygen can act as the master regulator of the relative sensitivity of the cytochrome c oxidase and sGC signalling pathways to NO. These findings have important implications for our understanding of the interplay between NO and oxygen in both physiology and the pathology of diseases associated with hypoxia.Key words: cytochrome c oxidase, haem (heme), mitochondria, nitric oxide, redox signalling.Nitric oxide (NO) is an unusual signalling molecule since its biological responses are primarily governed by its chemical reactivity [1]. In fact, the first signalling function of NO was revealed with the discovery that NO serves as a ligand for the haem group in sGC (soluble guanylate cyclase), resulting in increased cGMP production and activation of downstream signalling cascades. However, the story became more complex with the recognition that NO serves as a ligand for other haem proteins such as COX (cytochrome c oxidase) in the mitochondria and haemoglobin in the red blood cell [2,3]. The fact that NO interacts with the haem groups that normally bind oxygen essentially expanded the role of NO in cell signalling from a simple haem ligand to a regulatory modulator of oxygen-sensitive processes [4][5][6].Since both COX and sGC frequently co-exist within the same cell, the relative sensitivity of the two pathways to NO should determine the ultimate biological effect. It has been shown that activation of sGC occurs at much lower concentrations of NO than inhibition of COX, but these studies have not addressed the sensitivity of these pathways using endogenous NO formation; nor have they investigated the influence of oxygen on this relative sensitivity in a cellular setting [7]. Using an elegant experimental model that allows the controlled formation of NO from iNOS (inducible NO synthase) in cells that contain both COX and sGC, the authors have compared the response of these two signalling pathways with the concentration of NO measured extracellularly. Several endpoints were selected to assess the activity of sGC and COX. These include production of cGMP and phosphorylation of VASP (vasodilator-stimulated phosphoprotein) for the sGC pathway, and oxygen consumption and AMPK (AMP-activated protein kinase) phosphorylation for the COX pathway. The acti...

show abstract

Nitric oxide: orchestrating hypoxia regulation through mitochondrial respiration and the endoplasmic reticulum stress response

Cited by 78 publications

References 16 publications

Ultrastructure and histochemistry of rat myocardial capillary endothelial cells in response to diabetes and hypertension

Ultrastructure and histochemistry of rat myocardial capillary endothelial cells in response to diabetes and hypertension

Neuronal Nitric Oxide Synthase Plays a Key Role in CNS Demyelination

Evidence for oxygen as the master regulator of the responsiveness of soluble guanylate cyclase and cytochrome c oxidase to nitric oxide

Contact Info

Product

Resources

About