TY - JOUR
T1 - Clinical Pattern of Tolvaptan-Associated Liver Injury in Trial Participants With Autosomal Dominant Polycystic Kidney Disease (ADPKD)
T2 - An Analysis of Pivotal Clinical Trials
AU - Alpers, David H.
AU - Lewis, James H.
AU - Hunt, Christine M.
AU - Freston, James W.
AU - Torres, Vicente E.
AU - Li, Hui
AU - Wang, Wenchyi
AU - Hoke, Molly E.
AU - Roth, Sharin E.
AU - Westcott-Baker, Lucas
AU - Estilo, Alvin
N1 - Funding Information:
The trials analyzed here and retrospective safety analysis were supported by Otsuka Pharmaceutical Development & Commercialization (Rockville, MD). The sponsor participated in the design of the study; collection, analysis, and interpretation of data; writing the report; and the decision to submit the report for publication. Alice Walton, PhD, and Andrew Horgan, PhD, of BioScience Communications, Inc (New York, NY) assisted in drafting the manuscript, activity that was also funded by Otsuka. Each author participated in decisions on which data and outcomes were to be reported and in the interpretation of the data and the conclusions to be drawn.
Funding Information:
David H. Alpers, MD, James H. Lewis, MD, Christine M. Hunt, MD, MPH, James W. Freston, MD, PhD, Vicente E. Torres, MD, PhD, Hui Li, MS, Wenchyi Wang, PhD, Molly E. Hoke, PhD, Sharin E. Roth, MS, Lucas Westcott-Baker, MS, and Alvin Estilo, MD. Data acquisition: MEH, SER, AE; data analysis/interpretation: DHA, JHL, CMH, JWF, VET, HL, WW, MEH, SER, LW-B, AE; statistical analysis: HL, WW. Each author contributed important intellectual content during manuscript drafting or revision and agrees to be personally accountable for the individual's own contributions and to ensure that questions pertaining to the accuracy or integrity of any portion of the work, even one in which the author was not directly involved, are appropriately investigated and resolved, including with documentation in the literature if appropriate. The trials analyzed here and retrospective safety analysis were supported by Otsuka Pharmaceutical Development & Commercialization (Rockville, MD). The sponsor participated in the design of the study; collection, analysis, and interpretation of data; writing the report; and the decision to submit the report for publication. Alice Walton, PhD, and Andrew Horgan, PhD, of BioScience Communications, Inc (New York, NY) assisted in drafting the manuscript, activity that was also funded by Otsuka. Each author participated in decisions on which data and outcomes were to be reported and in the interpretation of the data and the conclusions to be drawn. Drs Alpers, Lewis, and Hunt are paid consultants to Otsuka. Drs Alpers, Lewis, Hunt, and Freston are members of the HAC for tolvaptan, which is sponsored by Otsuka. Dr Alpers is the chair and Drs Lewis, Hunt, and Freston are members of the HAC for the phase 3 ALERT trial for lixivaptan, which is sponsored by Palladio Biosciences. Dr Hunt also reports consulting for Galmed and Akebia Therapeutics Inc. Dr Torres reports grants from Otsuka Pharmaceutical, Palladio Biosciences, Sanofi Genzyme, Blueprint Medicines, and Mironid outside the submitted work. Dr Wang, Ms Li, Ms Roth, Mr Westcott-Baker, and Dr Estilo are employees of Otsuka. Dr Hoke is a former employee of Otsuka. The authors thank Peter C. Harris, PhD, of Mayo Clinic (Rochester, MN) for generating the PKD1/PKD2 genotyping data. To submit inquiries related to Otsuka clinical research, or to request access to individual participant data (IPD) associated with any Otsuka clinical trial, please visit https://clinical-trials.otsuka.com/. For all approved IPD access requests, Otsuka will share anonymized IPD on a remotely accessible data sharing platform. Received March 2, 2022. Evaluated by 2 external peer reviewers and a methods reviewer, with direct editorial input from an Associate Editor and the Editor-in-Chief. Accepted in revised form August 6, 2022.
Publisher Copyright:
© 2022 The Authors
PY - 2023/3
Y1 - 2023/3
N2 - Rationale & Objective: Tolvaptan is associated with risk of drug-induced liver injury when used to treat autosomal dominant polycystic kidney disease (ADPKD). After this risk was described based on the clinical trials TEMPO 3:4 and TEMPO 4:4, additional data from the REPRISE trial and a long-term extension of TEMPO 4:4, REPRISE, and other tolvaptan trials in ADPKD have become available. To further characterize the hepatic safety profile of tolvaptan, an analysis of the expanded dataset was conducted. Study Design: Analysis of safety data from prospective clinical trials of tolvaptan. Setting & Participants: Multicenter clinical trials including more than 2,900 tolvaptan-treated participants, more than 2,300 with at least 18 months of drug exposure. Intervention: Tolvaptan administered twice daily in split-dose regimens. Outcomes: Frequency of liver enzyme level increases detected by regular laboratory monitoring. Results: In the placebo-controlled REPRISE trial, more tolvaptan- than placebo-treated participants (38 of 681 [5.6%] vs 8 of 685 [1.2%]) experienced alanine aminotransferase level increases to >3× the upper limit of normal (ULN), similar to TEMPO 3:4 (40 of 957 [4.4%] vs 5 of 484 [1.0%]). No participant in REPRISE or the long-term extension experienced concurrent alanine aminotransferase level increases to >3× ULN and total bilirubin increases to >2× ULN (“Hy's Law” laboratory criteria). Based on the expanded dataset, liver enzyme increases most often occurred within 18 months after tolvaptan initiation and were less frequent thereafter. Increased levels returned to normal or near normal after treatment interruption or discontinuation. Thirty-eight patients were rechallenged with tolvaptan after the initial drug-induced liver injury episode, with return of liver enzyme level increases in 30; 1 additional participant showed a clinical “adaptation” after the initial episode, with resolution of the enzyme level increases despite continuation of tolvaptan. Limitations: Retrospective analysis. Conclusions: The absence of Hy's Law cases in REPRISE and the long-term extension trial support monthly liver enzyme monitoring during the first 18 months of tolvaptan exposure and every 3 months thereafter to detect and manage enzyme level increases, as is recommended on the drug label. Funding: Otsuka Pharmaceutical Development & Commercialization, Inc. Trial Registration: Trials included in the dataset were registered at ClinicalTrials.gov with study numbers NCT00428948 (TEMPO 3:4), NCT01214421 (TEMPO 4:4), NCT02160145 (REPRISE), and NCT02251275 (long-term extension).
AB - Rationale & Objective: Tolvaptan is associated with risk of drug-induced liver injury when used to treat autosomal dominant polycystic kidney disease (ADPKD). After this risk was described based on the clinical trials TEMPO 3:4 and TEMPO 4:4, additional data from the REPRISE trial and a long-term extension of TEMPO 4:4, REPRISE, and other tolvaptan trials in ADPKD have become available. To further characterize the hepatic safety profile of tolvaptan, an analysis of the expanded dataset was conducted. Study Design: Analysis of safety data from prospective clinical trials of tolvaptan. Setting & Participants: Multicenter clinical trials including more than 2,900 tolvaptan-treated participants, more than 2,300 with at least 18 months of drug exposure. Intervention: Tolvaptan administered twice daily in split-dose regimens. Outcomes: Frequency of liver enzyme level increases detected by regular laboratory monitoring. Results: In the placebo-controlled REPRISE trial, more tolvaptan- than placebo-treated participants (38 of 681 [5.6%] vs 8 of 685 [1.2%]) experienced alanine aminotransferase level increases to >3× the upper limit of normal (ULN), similar to TEMPO 3:4 (40 of 957 [4.4%] vs 5 of 484 [1.0%]). No participant in REPRISE or the long-term extension experienced concurrent alanine aminotransferase level increases to >3× ULN and total bilirubin increases to >2× ULN (“Hy's Law” laboratory criteria). Based on the expanded dataset, liver enzyme increases most often occurred within 18 months after tolvaptan initiation and were less frequent thereafter. Increased levels returned to normal or near normal after treatment interruption or discontinuation. Thirty-eight patients were rechallenged with tolvaptan after the initial drug-induced liver injury episode, with return of liver enzyme level increases in 30; 1 additional participant showed a clinical “adaptation” after the initial episode, with resolution of the enzyme level increases despite continuation of tolvaptan. Limitations: Retrospective analysis. Conclusions: The absence of Hy's Law cases in REPRISE and the long-term extension trial support monthly liver enzyme monitoring during the first 18 months of tolvaptan exposure and every 3 months thereafter to detect and manage enzyme level increases, as is recommended on the drug label. Funding: Otsuka Pharmaceutical Development & Commercialization, Inc. Trial Registration: Trials included in the dataset were registered at ClinicalTrials.gov with study numbers NCT00428948 (TEMPO 3:4), NCT01214421 (TEMPO 4:4), NCT02160145 (REPRISE), and NCT02251275 (long-term extension).
KW - alanine aminotransferase (ALT)
KW - aspartate aminotransferase (AST)
KW - Autosomal dominant polycystic kidney disease (ADPKD)
KW - clinical trial
KW - drug rechallenge
KW - drug-induced liver injury (DILI)
KW - hepatic events
KW - Hy's Law
KW - JYNARQUE
KW - liver safety
KW - tolvaptan
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U2 - 10.1053/j.ajkd.2022.08.012
DO - 10.1053/j.ajkd.2022.08.012
M3 - Article
C2 - 36191725
AN - SCOPUS:85147910448
SN - 0272-6386
VL - 81
SP - 281-293.e1
JO - American Journal of Kidney Diseases
JF - American Journal of Kidney Diseases
IS - 3
ER -