TASK−/− mice produce excess aldosterone and exhibit characteristics of idiopathic primary hyperaldosteronism. Twenty-four-hour urine chemistries after 1 week on sodium diets were as follows: low Na (LS, 0.05%), normal Na (NS, 0.32%), high Na (HS, 4%). Mice were studied (n = 10/genotype) in metabolic cages (7 days per diet): control (open circles) and TASK−/− (filled circles). (A) Urinary aldosterone (Ualdosterone) normalized to creatinine (†, genotype main effect, F1,18 = 10.03, P < 0.005) and plasma renin (†, F1,11 = 11.2, P < 0.005). (B) Urinary aldosterone for each animal on HS, normalized to NS. Circles, mean values ± SEM on days 4–7 of HS; squares, mean of each genotype (n = 10). (C) Time course of urinary aldosterone on HS after LS (†, F1,18 = 12.45, P < 0.002). (D) Time course of urinary aldosterone after candesartan administration to mice on LS (†, F1,4 = 8.53, P < 0.05). (E) Steady-state urinary aldosterone (†, F1,4 = 39.15, P < 0.005) and plasma renin (†, F1,4 = 39.1, P < 0.005) expressed relative to control animals on NS diet; genotype differences are independent of treatment. (F) Urinary Na and K are not different between genotypes on any diet. (†, F value for genotype main effect by two-way RM-ANOVA; *, P < 0.05, control vs. TASK−/− on indicated treatment, Student–Neuman–Keuls post hoc test).