4.7 Article

Sex and SP-A2 Dependent NAD(H) Redox Alterations in Mouse Alveolar Macrophages in Response to Ozone Exposure: Potential Implications for COVID-19

Journal

ANTIOXIDANTS
Volume 9, Issue 10, Pages -

Publisher

MDPI
DOI: 10.3390/antiox9100915

Keywords

optical redox imaging; nicotinamide adenine dinucleotide (NAD(H)); oxidized flavoprotein containing flavin adenine dinucleotide (FAD); redox ratio; surfactant protein A2 (SP-A2); surfactant protein A; macrophage activation; ozone; redox heterogeneity; innate immunity; lung

Funding

  1. CHILD Research Fund Department of Pediatrics, Pennsylvania State University College of Medicine
  2. NIH [R01CA191207]

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Co-enzyme nicotinamide adenine dinucleotide (NAD(H)) redox plays a key role in macrophage function. Surfactant protein (SP-) A modulates the functions of alveolar macrophages (AM) and ozone (O-3) exposure in the presence or absence of SP-A and reduces mouse survival in a sex-dependent manner. It is unclear whether and how NAD(H) redox status plays a role in the innate immune response in a sex-dependent manner. We investigated the NAD(H) redox status of AM from SP-A2 and SP-A knockout (KO) mice in response to O-3 or filtered air (control) exposure using optical redox imaging technique. We found: (i) In SP-A2 mice, the redox alteration of AM in response to O-3 showed sex-dependence with AM from males being significantly more oxidized and having a higher level of mitochondrial reactive oxygen species than females; (ii) AM from KO mice were more oxidized after O-3 exposure and showed no sex differences; (iii) AM from female KO mice were more oxidized than female SP-A2 mice; and (iv) Two distinct subpopulations characterized by size and redox status were observed in a mouse AM sample. In conclusions, the NAD(H) redox balance in AM responds to O-3 in a sex-dependent manner and the innate immune molecule, SP-A2, contributes to this observed sex-specific redox response.

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