Nitric oxide, cytochrome c and mitochondria

1999 ◽  
Vol 66 ◽  
pp. 17-25 ◽  
Author(s):  
Guy C. Brown ◽  
Vilmante Borutaite
Keyword(s):  
Nitric Oxide ◽  
Hydrogen Peroxide ◽  
Cytochrome C ◽  
Cytochrome Oxidase ◽  
Protease Activity ◽  
Complex I ◽  
Glutamate Release ◽  
Nerve Terminals ◽  
No Inhibition ◽  
Brain Nerve Terminals

Nitric oxide (NO) and its derivative, peroxynitrite (ONOO-), inhibit mitochondrial respiration, and this inhibition may contribute to both the physiological and cytotoxic actions of NO. Nanomolar concentrations of NO rapidly and reversibly inhibited cytochrome oxidase in competition with oxygen, as shown with isolated cytochrome oxidase, mitochondria, brain nerve terminals and cells. Cultured astrocytes and macrophages activated (by cytokines and endotoxin) to express the inducible form of NO synthase produced up to 1 μM NO, and inhibited their own respiration and that of co-incubated cells via reversible NO inhibition of cytochrome oxidase. NO-induced inhibition of respiration in brain nerve terminals resulted in rapid glutamate release, which might contribute to the neurotoxicity of NO. NO inhibition of cytochrome oxidase is reversible; however, incubation of cells with NO donors for 4 hours resulted in an inhibition of complex I, which was reversible by light and thiol reagents and may be due to nitrosylation of thiols in complex I. NO also caused the acute inhibition of catalase, stimulation of hydrogen peroxide production by mitochondria, and reaction with hydrogen peroxide on superoxide dismutase to produce peroxynitrite. Peroxynitrite inhibited complexes I, II and V (the ATP synthase), aconitase, creatine kinase, and increases the proton leak in isolated mitochondria. Peroxynitrite also caused opening of the permeability transition pore, resulting in the release of cytochrome c, which might then trigger apoptosis. Hypoxia/ischaemia also resulted in an acute reversible inhibition of cytochrome oxidase. Heart ischaemia caused the release of cytochrome c from mitochondria into the cytosol, and at the same time caspase-3-like-protease activity was activated in the cytoplasm. Addition of cytochrome c to non-ischaemic cytosol also caused activation of this protease activity, suggesting that caspase activation and consequent apoptosis is at least partly a result of this cytochrome c release.

Nitric oxide regulation of mitochondrial oxygen consumption II: molecular mechanism and tissue physiology

2007 ◽  
Vol 292 (6) ◽  
pp. C1993-C2003 ◽  
Author(s):  
Chris E. Cooper ◽  
Cecilia Giulivi
Keyword(s):  
Nitric Oxide ◽  
Oxygen Consumption ◽  
Cytochrome C ◽  
Cytochrome Oxidase ◽  
Molecular Mechanism ◽  
Guanylate Cyclase ◽  
Redox State ◽  
Physiological Role ◽  
Metabolic Effects ◽  
Whole Body

Nitric oxide (NO) is an intercellular signaling molecule; among its many and varied roles are the control of blood flow and blood pressure via activation of the heme enzyme, soluble guanylate cyclase. A growing body of evidence suggests that an additional target for NO is the mitochondrial oxygen-consuming heme/copper enzyme, cytochrome c oxidase. This review describes the molecular mechanism of this interaction and the consequences for its likely physiological role. The oxygen reactive site in cytochrome oxidase contains both heme iron ( a3) and copper (CuB) centers. NO inhibits cytochrome oxidase in both an oxygen-competitive (at heme a3) and oxygen-independent (at CuB) manner. Before inhibition of oxygen consumption, changes can be observed in enzyme and substrate (cytochrome c) redox state. Physiological consequences can be mediated either by direct “metabolic” effects on oxygen consumption or via indirect “signaling” effects via mitochondrial redox state changes and free radical production. The detailed kinetics suggest, but do not prove, that cytochrome oxidase can be a target for NO even under circumstances when guanylate cyclase, its primary high affinity target, is not fully activated. In vivo organ and whole body measures of NO synthase inhibition suggest a possible role for NO inhibition of cytochrome oxidase. However, a detailed mapping of NO and oxygen levels, combined with direct measures of cytochrome oxidase/NO binding, in physiology is still awaited.

scholarly journals Complex I and cytochrome c are molecular targets of flavonoids that inhibit hydrogen peroxide production by mitochondria

2011 ◽  
Vol 1807 (12) ◽  
pp. 1562-1572 ◽  
Author(s):  
Ricardo Lagoa ◽  
Ilaria Graziani ◽  
Carmen Lopez-Sanchez ◽  
Virginio Garcia-Martinez ◽  
Carlos Gutierrez-Merino
Keyword(s):  
Hydrogen Peroxide ◽  
Cytochrome C ◽  
Complex I ◽  
Molecular Targets ◽  
Hydrogen Peroxide Production

scholarly journals (+)-Catechin inhibits heart mitochondrial complex I and nitric oxide synthase: functional consequences on membrane potential and hydrogen peroxide production

2019 ◽  
Vol 10 (5) ◽  
pp. 2528-2537 ◽  
Author(s):  
Darío E. Iglesias ◽  
Silvina S. Bombicino ◽  
Alberto Boveris ◽  
Laura B. Valdez
Keyword(s):  
Nitric Oxide ◽  
Hydrogen Peroxide ◽  
Membrane Potential ◽  
Complex I ◽  
Mitochondrial Complex I ◽  
Mitochondrial Complex ◽  
Hydrogen Peroxide Production ◽  
Functional Consequences ◽  
Oxide Synthase

The aim was to study thein vitroeffect of nM to low μM concentration of (+)-catechin on the enzymatic activities of mitochondrial complex I and mtNOS, as well as the consequences on the membrane potential and H2O2production rate.

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