Short‐ and long‐term treatment of dilutional hyponatraemia with satavaptan, a selective arginine vasopressin V 2 ‐receptor antagonist: the DILIPO study

Aims Arginine vasopressin (AVP) V 2 receptor antagonism is a new approach to the management of hyponatraemia in congestive heart failure (CHF). The aim of this study was to investigate the efficacy and safety of satavaptan, an oral AVP V 2 ‐receptor antagonist, in patients with dilutional hyponatraemia. Methods and results A total of 118 patients (90 with CHF) with dilutional hyponatraemia (serum sodium 115–132 mmol/L) were randomized to double‐blind treatment with placebo or to 25 or 50 mg/day of satavaptan for 4 days, followed by non‐comparative open‐label satavaptan therapy for up to 343 days. The response rate (sodium ≥135 mmol/L and/or an increase in ≥5 mmol/L above baseline) was significantly higher with satavaptan 50 mg than with placebo (61.0 vs. 26.8%; P = 0.0035), with a trend towards significance with satavaptan 25 mg (48.6%, P = 0.0599). Median times to response were 3.30 and 2.79 days with satavaptan 25 and 50 mg/day, respectively, both shorter than placebo (>4 days; P = 0.0278 and P = 0.0004, respectively). Satavaptan therapy was effective in CHF patients, with response rates higher with both satavaptan 25 mg/day (53.6%) and 50 mg/day (57.1%) than with placebo (23.5%; P = 0.019 and P = 0.009, respectively). Sodium responses were maintained during open‐label therapy after a temporary study drug discontinuation period. Higher rates of adverse events occurred with the 50 mg/day dose, including rapid correction of hyponatraemia. Conclusions In patients with dilutional hyponatraemia, V 2 receptor antagonism with satavaptan was effective in increasing serum sodium concentrations. The long‐term open‐label treatment results demonstrate sustained efficacy of satavaptan in maintaining normal sodium levels. Trial Registration clinicaltrials.gov Identifier: NCT00274326