Abstract
BackgroundHyperoxia is a well-known cause of cerebral white matter injury in preterm infants with male sex being an independent and critical risk factor for poor neurodevelopmental outcome. Sex is therefore being widely considered as one of the major decisive factors for prognosis and treatment of these infants. But unfortunately, we still lack a clear view of the molecular mechanisms that lead to such a profound difference. Hence, using mouse-derived primary oligodendrocyte progenitor cells (OPCs), we investigated the molecular factors and underlying mechanisms behind the differential response of male and female cells towards oxidative stress.ResultsWe demonstrate that oxidative stress severely affects cellular functions related to energy metabolism, stress response, and maturation in the male-derived OPCs, whereas the female cells remain largely unaffected. CNPase protein level was found to decline following hyperoxia in male but not in female cells. This impairment of maturation was accompanied by the downregulation of nucleoporin and nuclear lamina proteins in the male cells. We identify Nup133 as a novel target protein affected by hyperoxia, whose inverse regulation may mediate this differential response in the male and female cells. Nup133 protein level declined following hyperoxia in male but not in female cells. We show that nuclear respiratory factor 1 (Nrf1) is a direct downstream target of Nup133 and that Nrf1 mRNA declines following hyperoxia in male but not in female cells. The female cells may be rendered resistant due to synergistic protection via the estrogen receptor alpha (ERα) which was upregulated following hyperoxia in female but not in male cells. Both Nup133 and ERα regulate mitochondrial function and oxidative stress response by transcriptional regulation of Nrf1.ConclusionsThese findings from a basic cell culture model establish prominent sex-based differences and suggest a novel mechanism involved in the differential response of OPCs towards oxidative stress. It conveys a strong message supporting the need to study how complex cellular processes are regulated differently in male and female brains during development and for a better understanding of how the brain copes up with different forms of stress after preterm birth.
Highlights
Hyperoxia is a well-known cause of cerebral white matter injury in preterm infants with male sex being an independent and critical risk factor for poor neurodevelopmental outcome
Hyperoxia leads to impairment of differentiation and disrupts mitochondrial function and stress response pathways in male Oligodendrocyte precursor cell (OPC) We tested different concentrations and time periods of oxygen treatment to find an optimum that allowed us to identify the initial target proteins affected by hyperoxia whose effect could be otherwise masked by the later response of large number of proteins responding to widespread severe oxidative stress and cell death
Giving a very clear picture of the impact of hyperoxia on different molecular functions; these results indicate that the downregulation of these stress response pathways and extensive mitochondrial dysfunction might be critical reasons behind a stronger negative effect on the male cells
Summary
Hyperoxia is a well-known cause of cerebral white matter injury in preterm infants with male sex being an independent and critical risk factor for poor neurodevelopmental outcome. Oxygen is considered as a major cause of perinatal insult to the developing brain in preterm infants leading to widespread white matter injury [6,7,8]. The fact that in most of the cases, preterm infants are born with immature lungs complicates the situation further They are frequently exposed to increased oxidative stress because of the use of supplemental oxygen often for a long period of time in resuscitation and treatment of neonatal lung diseases [9, 10]. The molecular mechanisms and details need to be still uncovered
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