Mitochondrial Complex IV Subunit 4 Isoform 2 Is Essential for Acute Pulmonary Oxygen Sensing

Natascha Sommer; Maik Hüttemann; Oleg Pak; Susan Scheibe; Fenja Knoepp; Christopher Sinkler; Monika Malczyk; Mareike Gierhardt; Azadeh Esfandiary; Simone Kraut; Felix Jonas; Christine Veith; Siddhesh Aras; Akylbek Sydykov; Nasim Alebrahimdehkordi; Klaudia Giehl; Matthias Hecker; Ralf P Brandes; Werner Seeger; Friedrich Grimminger; Hossein A Ghofrani; Ralph T Schermuly; Lawrence I Grossman; Norbert Weissmann

doi:10.1161/CIRCRESAHA.116.310482

Mitochondrial Complex IV Subunit 4 Isoform 2 Is Essential for Acute Pulmonary Oxygen Sensing

Circ Res. 2017 Aug 4;121(4):424-438. doi: 10.1161/CIRCRESAHA.116.310482. Epub 2017 Jun 15.

Authors

Natascha Sommer¹, Maik Hüttemann¹, Oleg Pak¹, Susan Scheibe¹, Fenja Knoepp¹, Christopher Sinkler¹, Monika Malczyk¹, Mareike Gierhardt¹, Azadeh Esfandiary¹, Simone Kraut¹, Felix Jonas¹, Christine Veith¹, Siddhesh Aras¹, Akylbek Sydykov¹, Nasim Alebrahimdehkordi¹, Klaudia Giehl¹, Matthias Hecker¹, Ralf P Brandes¹, Werner Seeger¹, Friedrich Grimminger¹, Hossein A Ghofrani¹, Ralph T Schermuly¹, Lawrence I Grossman², Norbert Weissmann¹

Affiliations

¹ From the Excellence Cluster Cardiopulmonary System, University of Giessen and Marburg Lung Center (UGMLC), Member of the German Center for Lung Research (DZL), Justus-Liebig-University, Giessen, Germany (N.S., O.P., S.S., F.K., M.M., M.G., A.E., S.K., F.J., C.V., A.S., N.A., K.G., M.H., W.S., F.G., H.A.G., R.T.S., N.W.); Center for Molecular Medicine and Genetics, Wayne State University School of Medicine, Detroit, MI (M.H., C.S., S.A., L.I.G.); Institut für Kardiovaskuläre Physiologie, Goethe-Universität, German Center for Cardiovascular Research (DZHK), Partner Site RheinMain, Frankfurt am Main, Germany (R.P.B.); and Max Planck Institute for Heart and Lung Research, Bad Nauheim, Germany (W.S.).
² From the Excellence Cluster Cardiopulmonary System, University of Giessen and Marburg Lung Center (UGMLC), Member of the German Center for Lung Research (DZL), Justus-Liebig-University, Giessen, Germany (N.S., O.P., S.S., F.K., M.M., M.G., A.E., S.K., F.J., C.V., A.S., N.A., K.G., M.H., W.S., F.G., H.A.G., R.T.S., N.W.); Center for Molecular Medicine and Genetics, Wayne State University School of Medicine, Detroit, MI (M.H., C.S., S.A., L.I.G.); Institut für Kardiovaskuläre Physiologie, Goethe-Universität, German Center for Cardiovascular Research (DZHK), Partner Site RheinMain, Frankfurt am Main, Germany (R.P.B.); and Max Planck Institute for Heart and Lung Research, Bad Nauheim, Germany (W.S.). lgrossman@wayne.edu Norbert.Weissmann@innere.med.uni-giessen.de.

Abstract

Rationale: Acute pulmonary oxygen sensing is essential to avoid life-threatening hypoxemia via hypoxic pulmonary vasoconstriction (HPV) which matches perfusion to ventilation. Hypoxia-induced mitochondrial superoxide release has been suggested as a critical step in the signaling pathway underlying HPV. However, the identity of the primary oxygen sensor and the mechanism of superoxide release in acute hypoxia, as well as its relevance for chronic pulmonary oxygen sensing, remain unresolved.

Objectives: To investigate the role of the pulmonary-specific isoform 2 of subunit 4 of the mitochondrial complex IV (Cox4i2) and the subsequent mediators superoxide and hydrogen peroxide for pulmonary oxygen sensing and signaling.

Methods and results: Isolated ventilated and perfused lungs from Cox4i2^-/- mice lacked acute HPV. In parallel, pulmonary arterial smooth muscle cells (PASMCs) from Cox4i2^-/- mice showed no hypoxia-induced increase of intracellular calcium. Hypoxia-induced superoxide release which was detected by electron spin resonance spectroscopy in wild-type PASMCs was absent in Cox4i2^-/- PASMCs and was dependent on cysteine residues of Cox4i2. HPV could be inhibited by mitochondrial superoxide inhibitors proving the functional relevance of superoxide release for HPV. Mitochondrial hyperpolarization, which can promote mitochondrial superoxide release, was detected during acute hypoxia in wild-type but not Cox4i2^-/- PASMCs. Downstream signaling determined by patch-clamp measurements showed decreased hypoxia-induced cellular membrane depolarization in Cox4i2^-/- PASMCs compared with wild-type PASMCs, which could be normalized by the application of hydrogen peroxide. In contrast, chronic hypoxia-induced pulmonary hypertension and pulmonary vascular remodeling were not or only slightly affected by Cox4i2 deficiency, respectively.

Conclusions: Cox4i2 is essential for acute but not chronic pulmonary oxygen sensing by triggering mitochondrial hyperpolarization and release of mitochondrial superoxide which, after conversion to hydrogen peroxide, contributes to cellular membrane depolarization and HPV. These findings provide a new model for oxygen-sensing processes in the lung and possibly also in other organs.

Keywords: electron transport complex IV; hypoxia; mitochondria; potassium channels; pulmonary circulation; reactive oxygen species.

MeSH terms

Animals
Cell Hypoxia / physiology
Cell Line, Tumor
Electron Transport Complex IV / genetics
Electron Transport Complex IV / metabolism*
Female
Humans
Lung / metabolism*
Male
Membrane Potential, Mitochondrial / physiology
Mice
Mice, Knockout
Mitochondria / genetics
Mitochondria / metabolism*
Oxygen / metabolism*

Substances

COX4I2 protein, human
Electron Transport Complex IV
Oxygen

Grants and funding

R01 GM048517/GM/NIGMS NIH HHS/United States