Attenuation of oxidative damage by targeting mitochondrial complex I in neonatal hypoxic-ischemic brain injury

Minso Kim; Anna Stepanova; Zoya Niatsetskaya; Sergey Sosunov; Sabine Arndt; Michael P Murphy; Alexander Galkin; Vadim S Ten

doi:10.1016/j.freeradbiomed.2018.06.040

Attenuation of oxidative damage by targeting mitochondrial complex I in neonatal hypoxic-ischemic brain injury

Free Radic Biol Med. 2018 Aug 20:124:517-524. doi: 10.1016/j.freeradbiomed.2018.06.040. Epub 2018 Jul 3.

Authors

Minso Kim¹, Anna Stepanova², Zoya Niatsetskaya¹, Sergey Sosunov¹, Sabine Arndt³, Michael P Murphy³, Alexander Galkin⁴, Vadim S Ten⁵

Affiliations

¹ Department of Pediatrics, Division of Neonatology, Columbia University, NY, USA.
² Department of Pediatrics, Division of Neonatology, Columbia University, NY, USA; School of Biological Sciences, Queen's University Belfast, UK.
³ MRC Mitochondrial Biology Unit, University of Cambridge, Cambridge, UK.
⁴ Department of Pediatrics, Division of Neonatology, Columbia University, NY, USA; School of Biological Sciences, Queen's University Belfast, UK. Electronic address: ag4003@cumc.columbia.edu.
⁵ Department of Pediatrics, Division of Neonatology, Columbia University, NY, USA. Electronic address: vt82@columbia.edu.

PMID: 30037775
PMCID: PMC6389362
DOI: 10.1016/j.freeradbiomed.2018.06.040

Abstract

Background: Establishing sustained reoxygenation/reperfusion ensures not only the recovery, but may initiate a reperfusion injury in which oxidative stress plays a major role. This study offers the mechanism and this mechanism-specific therapeutic strategy against excessive release of reactive oxygen species (ROS) associated with reperfusion-driven recovery of mitochondrial metabolism.

Aims and methods: In neonatal mice subjected to cerebral hypoxia-ischaemia (HI) and reperfusion, we examined conformational changes and activity of mitochondrial complex I with and without post-HI administration of S-nitrosating agent, MitoSNO. Assessment of mitochondrial ROS production, oxidative brain damage, neuropathological and neurofunctional outcomes were used to define neuroprotective strength of MitoSNO. A specificity of reperfusion-driven mitochondrial ROS production to conformational changes in complex I was examined in-vitro.

Results: HI deactivated complex I, changing its conformation from active form (A) into the catalytically dormant, de-active form (D). Reperfusion rapidly converted the D-form into the A-form and increased ROS generation. Administration of MitoSNO at the onset of reperfusion, decelerated D→A transition of complex I, attenuated oxidative stress, and significantly improved neurological recovery. In cultured neurons, after simulated ischaemia-reperfusion injury, MitoSNO significantly reduced ROS generation and neuronal mortality. In isolated mitochondria subjected to anoxia-reoxygenation, MitoSNO restricted ROS release during D→A transitions.

Conclusion: Rapid D→A conformation in response to reperfusion reactivates complex I. This is essential not only for metabolic recovery, but also contributes to excessive release of mitochondrial ROS and reperfusion injury. We propose that the initiation of reperfusion should be followed by pharmacologically-controlled gradual reactivation of complex I.

Keywords: Hypoxia/ischaemia; Ischaemia/reperfusion damage; Mitochondrial complex I; Nitrosation.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Animals, Newborn
Electron Transport Complex I / drug effects*
Electron Transport Complex I / metabolism*
Hypoxia-Ischemia, Brain / metabolism*
Mice
Mice, Inbred C57BL
Neuroprotective Agents / pharmacology*
Nitrosation / drug effects
Oxidative Stress / drug effects
Reactive Oxygen Species / metabolism
Reperfusion Injury / metabolism*

Substances

Neuroprotective Agents
Reactive Oxygen Species
Electron Transport Complex I

Abstract

Publication types

MeSH terms

Substances

Grants and funding