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Nup133 and ERα mediate the differential effects of hyperoxia-induced damage in male and female OPCs.

Donna Elizabeth SunnyElke HammerSebastian StrempelChristy JosephHimanshu ManchandaTill IttermannStephanie HübnerFrank Ulrich WeissUwe VölkerMatthias Heckmann
Published in: Molecular and cellular pediatrics (2020)
These 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.
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