Tolvaptan for Children and Adolescents with Autosomal Dominant Polycystic Kidney Disease: Randomized Controlled Trial

Overview

Journal Clin J Am Soc Nephrol

Specialty Nephrology

Date 2023 Jan 31

PMID 36719158

Authors

Djalila Mekahli

Lisa M Guay-Woodford

Melissa A Cadnapaphornchai

Larry A Greenbaum

Mieczyslaw Litwin

Tomas Seeman

Ann Dandurand

Lily Shi

Kimberly Sikes

Susan E Shoaf

Franz Schaefer

Affiliations

Soon will be listed here.

Abstract

Background: Tolvaptan slows expansion of kidney volume and kidney function decline in adults with autosomal dominant polycystic kidney disease (ADPKD). Progression during childhood could be treated before irreversible kidney damage occurs, but trial data are lacking. We evaluated the safety and efficacy of tolvaptan in children/adolescents with ADPKD.

Methods: This was the 1-year, randomized, double-blind, portion of a phase 3b, two-part trial being conducted at 20 academic pediatric nephrology centers. Key eligibility criteria were ADPKD and eGFR ≥60 ml/min per 1.73 m2. Participants aged 12-17 years were the target group (group 1, enrollment goal n≥60); participants aged 4-11 years could additionally enroll (group 2, anticipated enrollment approximately 40). Treatments were tolvaptan or placebo titrated by body weight and tolerability. Coprimary end points, change from baseline in spot urine osmolality and specific gravity at week 1, assessed inhibition of antidiuretic hormone activity. The key secondary end point was change in height-adjusted total kidney volume (htTKV) to month 12 in group 1. Additional end points were safety/tolerability and quality of life. Statistical comparisons were exploratory and post hoc.

Results: Among the 91 randomized (group 1, n=66; group 2, n=25), least squares (LS) mean reduction (±SEM) in spot urine osmolality at week 1 was greater with tolvaptan (-390 [28] mOsm/kg) than placebo (-90 [29] mOsm/kg; P<0.001), as was LS mean reduction in specific gravity (-0.009 [0.001] versus -0.002 [0.001]; P<0.001). In group 1, the 12-month htTKV increase was 2.6% with tolvaptan and 5.8% with placebo (P>0.05). For tolvaptan and placebo, respectively, 65% and 16% of subjects experienced aquaretic adverse events, and 2% and 0% experienced hypernatremia. There were no elevated transaminases or drug-induced liver injuries. Four participants discontinued tolvaptan, and three discontinued placebo. Quality-of-life assessments remained stable.

Conclusions: Tolvaptan exhibited pharmacodynamic activity in pediatric ADPKD. Aquaretic effects were manageable, with few discontinuations.

Clinical Trial Registry Name And Registration Number: Safety, Pharmacokinetics, Tolerability and Efficacy of Tolvaptan in Children and Adolescents With ADPKD (Autosomal Dominant Polycystic Kidney Disease) NCT02964273.

Citing Articles

Long-term tolvaptan therapy in a case of very early-onset polycystic kidney disease.

Joneliunaite V, Godron-Dubrasquet A, Allard L, Delmas J, Llanas B, Harambat J Pediatr Nephrol. 2025; .

PMID: 40025141 DOI: 10.1007/s00467-025-06732-2.

Commentary: Tolvaptan for Autosomal Dominant Polycystic Kidney Disease (ADPKD) - an update.

Gittus M, Haley H, Harris T, Borrows S, Padmanabhan N, Gale D BMC Nephrol. 2025; 26(1):79.

PMID: 39953521 PMC: 11827152. DOI: 10.1186/s12882-025-03960-4.

Safety and efficacy of tolvaptan in real‑world Japanese patients with autosomal dominant polycystic kidney disease: final results of SLOW‑PKD surveillance.

Mochizuki T, Muto S, Suzue K, Komaniwa S, Tanaka T, Fukuta Y Clin Exp Nephrol. 2025; .

PMID: 39953249 DOI: 10.1007/s10157-025-02634-7.

Characteristics of patients with autosomal polycystic kidney disease reaching kidney failure by age 40.

Wigerinck S, Schellekens P, Smith B, Hanna C, Dachy A, Chedid M Pediatr Nephrol. 2025; .

PMID: 39891678 DOI: 10.1007/s00467-024-06652-7.

Tolvaptan and Autosomal Dominant Polycystic Kidney Disease Progression in Individuals Aged 18-35 Years: A Pooled Database Analysis.

Chebib F, Dahl N, Zhou X, Garbinsky D, Wang J, Nunna S Kidney Med. 2025; 7(1):100935.

PMID: 39810815 PMC: 11731472. DOI: 10.1016/j.xkme.2024.100935.

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