Molecular Mechanisms of the Crosstalk Between Mitochondria and NADPH Oxidase Through Reactive Oxygen Species—Studies in White Blood Cells and in Animal Models

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RESEARCH PRODUCT

Molecular Mechanisms of the Crosstalk Between Mitochondria and NADPH Oxidase Through Reactive Oxygen Species—Studies in White Blood Cells and in Animal Models

Ning Xia Matthias Oelze Swenja Kröller-schön Nicolai Treiber Thomas Münzel Eberhard Schulz Huige Li Paul Stamm Yuliya Mikhed Philip Wenzel Sebastian Steven Karin Scharffetter-kochanek Elena Zinssius Andreas Daiber Alexander Scholz Sabine Kossmann Michael Mader Steffen Daub Michael Hausding

subject

Physiology Neutrophils Clinical Biochemistry Biology Mitochondrion medicine.disease_cause Biochemistry Models Biological Superoxide dismutase Cyclophilins Mice Forum Original Research CommunicationsMitochondria (A. Daiber Ed.)medicine Leukocytes Animals Humans Molecular Biology General Environmental Science Respiratory Burst chemistry.chemical_classification Mice Knockout Reactive oxygen species NADPH oxidase Superoxide Dismutase Angiotensin II NADPH Oxidases Biological Transport Cell Biology Respiratory burst Mitochondria Peroxides Enzyme Activation Crosstalk (biology)Oxidative Stress Mitochondrial permeability transition pore Biochemistry chemistry biology.protein cardiovascular system General Earth and Planetary Sciences Reactive Oxygen Species Oxidation-Reduction Oxidative stress Cyclophilin D

description

Aims: Oxidative stress is involved in the development of cardiovascular disease. There is a growing body of evidence for a crosstalk between different enzymatic sources of oxidative stress. With the present study, we sought to determine the underlying crosstalk mechanisms, the role of the mitochondrial permeability transition pore (mPTP), and its link to endothelial dysfunction. Results: NADPH oxidase (Nox) activation (oxidative burst and translocation of cytosolic Nox subunits) was observed in response to mitochondrial reactive oxygen species (mtROS) formation in human leukocytes. In vitro, mtROS-induced Nox activation was prevented by inhibitors of the mPTP, protein kinase C, tyrosine kinase cSrc, Nox itself, or an intracellular calcium chelator and was absent in leukocytes with p47phox deficiency (regulates Nox2) or with cyclophilin D deficiency (regulates mPTP). In contrast, the crosstalk in leukocytes was amplified by mitochondrial superoxide dismutase (type 2) (MnSOD+/−) deficiency. In vivo, increases in blood pressure, degree of endothelial dysfunction, endothelial nitric oxide synthase (eNOS) dysregulation/uncoupling (e.g., eNOS S-glutathionylation) or Nox activity, p47phox phosphorylation in response to angiotensin-II (AT-II) in vivo treatment, or the aging process were more pronounced in MnSOD+/− mice as compared with untreated controls and improved by mPTP inhibition by cyclophilin D deficiency or sanglifehrin A therapy. Innovation: These results provide new mechanistic insights into what extent mtROS trigger Nox activation in phagocytes and cardiovascular tissue, leading to endothelial dysfunction. Conclusions: Our data show that mtROS trigger the activation of phagocytic and cardiovascular NADPH oxidases, which may have fundamental implications for immune cell activation and development of AT-II-induced hypertension. Antioxid. Redox Signal. 20, 247–266.

year	journal	country	edition	language
2014-01-10

10.1089/ars.2012.4953 https://europepmc.org/articles/PMC3887465/