Your search keyword '"Elizabeth S. Hensen"' showing total 1 results

1. Misoprostol Treatment Prevents Hypoxia-Induced Cardiac Dysfunction Through a 14-3-3 and PKA regulatory motif on Bnip3

Author

Vernon W. Dolinsky, Richard Keijzer, Joseph W. Gordon, Nivedita Seshadri, Lucas Nguyen, Adrian R. West, Christine A. Doucette, Landon Falk, Jason Karch, Elizabeth S. Hensen, Ian M.C. Dixon, Sunil G. Rattan, Donald Chapman, Grant M. Hatch, Christof Rampitsch, Matthew D. Martens, Spencer B. Gibson, Bo Xiang, Arielys Mendoza, and Ayesha D Saleem

Subjects

Calcium metabolism, Ejection fraction, business.industry, Cell, Pharmacology, Hypoxia (medical), chemistry.chemical_compound, medicine.anatomical_structure, chemistry, Mitochondrial permeability transition pore, Medicine, Phosphorylation, medicine.symptom, business, Prostaglandin E1, Misoprostol, medicine.drug

Abstract

Systemic hypoxia is a common element in most perinatal emergencies and is a known driver of Bnip3 expression in the neonatal heart. Bnip3 plays a prominent role in the evolution of necrotic cell death, disrupting ER calcium homeostasis and initiating mitochondrial permeability transition (MPT). Emerging evidence suggests a cardioprotective role for the prostaglandin E1 analogue misoprostol during periods of hypoxia, but the mechanisms for this protection are not completely understood. Using a combination of mouse and cell models, we tested if misoprostol is cardioprotective during neonatal hypoxic injury by altering Bnip3 function. Here we report that hypoxia elicits mitochondrial-fragmentation, MPT, reduced ejection fraction, and evidence of necroinflammation, which were abrogated with misoprostol treatment or Bnip3 knockout. Through molecular studies we show that misoprostol leads to PKA-dependent Bnip3 phosphorylation at threonine-181, and subsequent redistribution of Bnip3 from mitochondrial Opa1 and the ER through an interaction with 14-3-3 proteins. Taken together, our results demonstrate a role for Bnip3 phosphorylation in the regulation of cardiomyocyte contractile/metabolic dysfunction, and necroinflammation. Furthermore, we identify a potential pharmacological mechanism to prevent neonatal hypoxic injury.

Published

2020