β3-adrenergic agonist counters oxidative stress and Na+-K+ pump inhibitory S-glutathionylation of placental cells: Implications for preeclampsia

Chia-Chi Liu; Yunjia Zhang; Yeon Jae Kim; Elisha J Hamilton; Bei Xu; Jane Limas; Sharon McCracken; Jonathan M Morris; Angela Makris; Annemarie Hennessy; Helge H Rasmussen

doi:10.1152/ajpcell.00379.2024

β3-adrenergic agonist counters oxidative stress and Na⁺-K⁺ pump inhibitory S-glutathionylation of placental cells: Implications for preeclampsia

Am J Physiol Cell Physiol. 2024 Nov 4. doi: 10.1152/ajpcell.00379.2024. Online ahead of print.

Authors

Affiliations

¹ Kolling Institute of Medical Research, University of Sydney, St. Leonards, NSW, Australia.
² The Heart Research Institute, Sydney, Australia.
³ University of Sydney, Sydney, Australia.
⁴ Kolling Institute of Medical Research, University of Sydney, Australia.
⁵ university of sydney, Australia.
⁶ University of Sydney, Australia.
⁷ University of Sydney, St Leonards, Australia.
⁸ Northern Sydney Local Health District, Australia.
⁹ Western Sydney University, Liverpool, Australia.
¹⁰ Vascular Immunology, The Heart Research Institute, campbelltown NSW, NSW, Australia.
¹¹ Department of Cardiology, Royal North Shore Hospital, Sydney, New South Wales, Australia.

PMID: 39495253
DOI: 10.1152/ajpcell.00379.2024

Abstract

Oxidative stress from placental ischemia/reperfusion and hypoxia/reoxygenation (H/R) in preeclampsia is accompanied by Na⁺-K⁺ pump inhibition and S-glutathionylation of its β1 subunit (GSS-β1), a modification that inhibits the pump. β3-adrenergic receptor (β3-AR) agonists can reverse GSS-β1. We examined effects of the agonist CL316,243 on GSS-β1 and sources of H/R-induced oxidative stress in immortalized first trimester human trophoblast (HTR-8/SVneo) and freshly isolated placental explants from normal term pregnancies. H/R increased GSS-β1 and, reflecting compromised α1/β1 subunit interaction, it reduced α1/β1 pump subunit co-immunoprecipitation. H/R increased p47^phox/p22^phox NADPH oxidase subunit co-immunoprecipitation reflecting membrane translocation of cytosolic p47^phox that is needed to activate NADPH oxidase. Fluorescence of O₂^•--sensitive dihydroethidium increased in parallel. H/R increased S-glutathionylation of endothelial nitric oxide synthase (GSS-eNOS) that uncouples NO synthesis towards synthesis of O₂^•- and reduced trophoblast migration. Oxidative stress induced by tumor necrosis factor α (TNF-α) increased soluble fms-like tyrosine kinase receptor 1 (sFlt-1) trophoblast release, a marker of preeclampsia, and reduced trophoblast integration into endothelial cellular networks. CL316,243 eliminated H/R-induced GSS-β1 and decreases of α1/β1 subunit coimmunoprecipitation, eliminated NADPH oxidase activation and increases in GSS-eNOS, restored trophoblast migration, eliminated increased sFlt-1 release and restored trophoblast integration in endothelial cell networks. H/R induced GSS-β1, α1/β1 subunit co-immunoprecipitation and NADPH oxidase activation of placental explants reflected effects of H/R for trophoblasts and CL316,243 eliminated these changes. We conclude a β3-AR agonist counters key pathophysiological features of preeclampsia in vitro. β3 agonists already in human use for another purpose are potential candidates for re-purposing to treat preeclampsia.

Keywords: Na+-K+ pump; Preeclampsia; S-glutathionylation; b3-adrenergic receptor; oxidative stress.

Grants and funding

Heart Research Australia (HRA)