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


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; Prss8cat/+ and Prss8cat/cat), and renal tubule-specific CAP1/Prss8 knockout (Prss8PaxLC1) 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 α- or γENaC subunit cleavage pattern did not differ from control mice. On standard and low Na+ diet, Prss8cat/+ and Prss8cat/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 (Prss8PaxLC1) 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.

SUBMITTER: Ehret E 

PROVIDER: S-EPMC9224322 | biostudies-literature | 2022 Jun

REPOSITORIES: biostudies-literature

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

Ehret Elodie E   Jäger Yannick Y   Sergi Chloé C   Mérillat Anne-Marie AM   Peyrollaz Thibaud T   Anand Deepika D   Wang Qing Q   Ino Fréderique F   Maillard Marc M   Kellenberger Stephan S   Gautschi Ivan I   Szabo Roman R   Bugge Thomas H TH   Vogel Lotte K LK   Hummler Edith E   Frateschi Simona S  

International journal of molecular sciences 20220616 12


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; <i>Prss8<sup>cat/+</sup></i> and <i>Prss8<sup>cat/cat</sup></i>), and renal tubule-specific CAP1/Prss8 knockout (Prss8<sup>PaxLC1</sup>) mice. When  ...[more]

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