Manganese superoxide dismutase and aldehyde dehydrogenase deficiency increase mitochondrial oxidative stress and aggravate age-dependent vascular dysfunction.

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RESEARCH PRODUCT

Manganese superoxide dismutase and aldehyde dehydrogenase deficiency increase mitochondrial oxidative stress and aggravate age-dependent vascular dysfunction.

Joachim Kienhöfer Andreas Daiber Eberhard Schulz Nicolai Treiber Thomas Münzel Alexander Bürkle Toshihiro Kawamoto Swenja Schuhmacher Matthias Oelze Marcus Hortmann Markus Bachschmid Johanna Müller Philip Wenzel Karin Scharffetter-kochanek

subject

Mitochondrial ROS Male Aging Physiology Vasodilator Agents Mitochondrion Vascular dysfunction medicine.disease_cause Mitochondria Heart Muscle Smooth Vascular chemistry.chemical_compound Mice Endothelial dysfunction Aorta chemistry.chemical_classification Mice Knockout biology Superoxide Aldehyde Dehydrogenase Mitochondrial Age Factors Vasodilation Biochemistry Cardiology and Cardiovascular Medicine Mitochondrial aldehyde dehydrogenase medicine.medical_specialty 8-oxodG Oxidative phosphorylation DNA Mitochondrial Superoxide dismutase Manganese superoxide dismutase ddc:570 Physiology (medical)Internal medicine medicine Animals Reactive oxygen species Dose-Response Relationship Drug Superoxide Dismutase Mitochondrial oxidative stress Original Articles Aldehyde Dehydrogenase medicine.disease Mice Inbred C57BL Oxidative Stress Endocrinology chemistry biology.protein Endothelium Vascular Reactive Oxygen Species Oxidative stress DNA Damage

description

AimsImbalance between pro- and antioxidant species (e.g. during aging) plays a crucial role for vascular function and is associated with oxidative gene regulation and modification. Vascular aging is associated with progressive deterioration of vascular homeostasis leading to reduced relaxation, hypertrophy, and a higher risk of thrombotic events. These effects can be explained by a reduction in free bioavailable nitric oxide that is inactivated by an age-dependent increase in superoxide formation. In the present study, mitochondria as a source of reactive oxygen species (ROS) and the contribution of manganese superoxide dismutase (MnSOD, SOD-2) and aldehyde dehydrogenase (ALDH-2) were investigated.Methods and resultsAge-dependent effects on vascular function were determined in aortas of C57/Bl6 wild-type (WT), ALDH-22/2, MnSOD+/+, and MnSOD+/ mice by isometric tension measurements in organ chambers. Mitochondrial ROS formation was measured by luminol (L-012)-enhanced chemiluminescence and 2-hydroxyethidium formation with an HPLC-based assay in isolatedheart mitochondria. ROS-mediated mitochondrial DNA (mtDNA) damage was detected by a novel and modified version of the fluorescent-detection alkaline DNA unwinding (FADU) assay. Endothelial dysfunction was observed in aged C57/Bl6 WT mice in parallel to increased mitochondrial ROS formation and oxidative mtDNA damage. In contrast, middle-aged ALDH-22/2 mice showed a marked vascular dysfunction that was similar in old ALDH-22/2 mice suggesting that ALDH-2 exerts agedependent vasoprotective effects. Aged MnSOD+/2 mice showed the most pronounced phenotype such as severely impaired vasorelaxation, highest levels of mitochondrial ROS formation and mtDNA damage.ConclusionThe correlation between mtROS formation and acetylcholine-dependent relaxation revealed that mitochondrial radical formation significantly contributes to age-dependent endothelial dysfunction.

year	journal	country	edition	language
2008-07-04	Cardiovascular research

10.1093/cvr/cvn182 https://pubmed.ncbi.nlm.nih.gov/18596060