Kidney-Specific CAP1/Prss8-Deficient Mice Maintain ENaC-Mediated Sodium Balance 
through an Aldosterone Independent Pathway

Ehret, Elodie; Jaeger, Yannick; Sergi, Chloe; Merillat, Anne-Marie; Peyrollaz, Thibaud; Anand, Deepika; Wang, Qing; Ino, Frederique; Maillard, Marc; Kellenberger, Stephan; Gautschi, Ivan; Szabo, Roman; Bugge, Thomas H.; Vogel, Lotte K.; Hummler, Edith; Frateschi, Simona

doi:10.3390/ijms23126745

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Kidney-Specific CAP1/Prss8-Deficient Mice Maintain ENaC-Mediated Sodium Balance through an Aldosterone Independent Pathway

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Jaeger, Yannick
Pharmacology, Max Planck Institute for Heart and Lung Research, Max Planck Society;

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Citation

Ehret, E., Jaeger, Y., Sergi, C., Merillat, A.-M., Peyrollaz, T., Anand, D., et al. (2022). Kidney-Specific CAP1/Prss8-Deficient Mice Maintain ENaC-Mediated Sodium Balance through an Aldosterone Independent Pathway. INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES, 23(12): 6745. doi:10.3390/ijms23126745.

Cite as: https://hdl.handle.net/21.11116/0000-000A-B000-E

Abstract

The serine protease prostasin (CAP1/Prss8, channel-activating protease-1) is a confirmed in vitro and in vivo activator of the epithelial sodium channel ENaC. To test whether proteolytic activity or CAP1/Prss8 abundance itself are required for ENaC activation in the kidney, we studied animals either hetero- or homozygous mutant at serine 238 (S238A; Prss8(cat/+) and Prss8(cat/cat)), and renal tubule-specific CAP1/Prss8 knockout (Prss8(PaxLC1)) mice. When exposed to varying Na+-containing diets, no changes in Na+ and K+ handling and only minor changes in the expression of Na+ and K+ transporting protein were found in both models. Similarly, the alpha- or gamma ENaC subunit cleavage pattern did not differ from control mice. On standard and low Na+ diet, Prss8(cat/+) and Prss8(cat/cat) mice exhibited standard plasma aldosterone levels and unchanged amiloride-sensitive rectal potential difference indicating adapted ENaC activity. Upon Na+ deprivation, mice lacking the renal CAP1/Prss8 expression (Prss8(PaxLC1)) exhibit significantly decreased plasma aldosterone and lower K+ levels but compensate by showing significantly higher plasma renin activity. Our data clearly demonstrated that the catalytic activity of CAP1/Prss8 is dispensable for proteolytic ENaC activation. CAP1/Prss8-deficiency uncoupled ENaC activation from its aldosterone dependence, but Na+ homeostasis is maintained through alternative pathways.