First Evidence for a Crosstalk Between Mitochondrial and NADPH Oxidase-Derived Reactive Oxygen Species in Nitroglycerin-Triggered Vascular Dysfunction

6533b871fe1ef96bd12d25c2

RESEARCH PRODUCT

First Evidence for a Crosstalk Between Mitochondrial and NADPH Oxidase-Derived Reactive Oxygen Species in Nitroglycerin-Triggered Vascular Dysfunction

Stephan Baldus Ralf P. Brandes Johanna Müller Thomas Münzel Swenja Schuhmacher Eberhard Schulz Andreas Daiber Tommaso Gori Matthias Oelze Hanke Mollnau Jennifer M. Dias Wickramanayake Philip Wenzel Marcus Hortmann

subject

Male Physiology Vasodilator Agents Clinical Biochemistry Mitochondrion Pharmacology medicine.disease_cause Biochemistry Mitochondria Heart Mice Nitroglycerin chemistry.chemical_compound Ethidium Aorta Chromatography High Pressure Liquid Heart metabolism General Environmental Science chemistry.chemical_classification NADPH oxidase biology Reverse Transcriptase Polymerase Chain Reaction Reactive Nitrogen Species Biochemistry Cyclosporine cardiovascular system circulatory and respiratory physiology Blotting Western In Vitro Techniques Transfection Cell Line Rotenone medicine Animals Humans RNA Messenger Rats Wistar Molecular Biology Reactive oxygen species NADPH Oxidases Cell Biology Rotenone Rats Mice Inbred C57BL chemistry Mitochondrial permeability transition pore Vasoconstriction Apocynin biology.protein General Earth and Planetary Sciences Reactive Oxygen Species Oxidative stress

description

Chronic nitroglycerin treatment results in development of nitrate tolerance associated with endothelial dysfunction (ED). We sought to clarify how mitochondria- and NADPH oxidase (Nox)-derived reactive oxygen species (ROS) contribute to nitrate tolerance and nitroglycerin-induced ED. Nitrate tolerance was induced by nitroglycerin infusion in male Wistar rats (100 microg/h/4 day) and in C57/Bl6, p47(phox/) and gp91(phox/) mice (50 microg/h/4 day). Protein and mRNA expression of Nox subunits were unaltered by chronic nitroglycerin treatment. Oxidative stress was determined in vascular rings and mitochondrial fractions of nitroglycerin-treated animals by L-012 enhanced chemiluminescence, revealing a dominant role of mitochondria for nitrate tolerance development. Isometric tension studies revealed that genetic deletion or inhibition (apocynin, 0.35 mg/h/4 day) of Nox improved ED, whereas nitrate tolerance was unaltered. Vice versa, nitrate tolerance was attenuated by co-treatment with the respiratory chain complex I inhibitor rotenone (100 microg/h/4 day) or the mitochondrial permeability transition pore blocker cyclosporine A (50 microg/h/4 day). Both compounds improved ED, suggesting a link between mitochondrial and Nox-derived ROS. Mitochondrial respiratory chain-derived ROS are critical for the development of nitrate tolerance, whereas Nox-derived ROS mediate nitrate tolerance-associated ED. This suggests a crosstalk between mitochondrial and Nox-derived ROS with distinct mechanistic effects and sites for pharmacological intervention.

year	journal	country	edition	language
2008-08-01	Antioxidants & Redox Signaling

https://doi.org/10.1089/ars.2007.1969