Determination of fasiglifam-induced liver toxicity: Insights from the data monitoring committee of the fasiglifam clinical trials program

Abstract

Background

Different approaches to safety event collection influence the determination of liver toxicity within drug development programs. Herein, a description of how fasiglifam-induced liver injury was detected is provided.

Methods

This eight-trial drug development program was intended to evaluate fasiglifam (25 mg, 50 mg) against placebo or active comparators (glimepiride, sitagliptin) in approximately 11,000 suboptimally controlled patients with type 2 diabetes (terminated Dec 2013 due to liver toxicity). Liver safety had been pre-identified as a concern, and within the phase 3 trials, was measured through (1) adverse event reporting, (2) central predefined liver monitoring schedule with various thresholds for potential drug-induced liver injury, and (3) blinded adjudication of serious liver toxicity by a panel of experts in drug-induced liver injury. A single data monitoring committee provided safety oversight across all trials within the program.

Findings

Prior to program termination, 7595 of 7602 (99.9%) randomized participants across the eight trials received at least one dose of the study drug (fasiglifam, placebo, or active control). No concerning trends were noted in adverse or serious adverse event frequency, suspected unexpected serious adverse reaction, alanine or aspartate transaminase elevations, or hepatobiliary or gastrointestinal adverse events as reported by local site investigators. However, the predefined central liver safety measurements revealed a greater frequency of possible Hy’s Law cases (5 vs 2) and a 3- to 7-fold greater relative risk in alanine or aspartate transaminase elevation (with respect to upper limit of normal) within fasiglifam recipients compared with placebo/active control: alanine or aspartate transaminase > 3×: relative risk 3.34 (95% confidence interval 2.29–4.90), alanine or aspartate transaminase > 5×: relative risk 6.60 (95% confidence interval 3.03–14.38), alanine or aspartate transaminase > 8×: relative risk 6.14 (95% confidence interval 2.18–17.27), and alanine or aspartate transaminase > 10×: relative risk 6.74 (95% confidence interval 2.05, 22.14). All elevations resolved on study drug discontinuation. Drug-induced liver injury was adjudicated as highly likely or probably related in 0.64% of fasiglifam-treated versus 0.06% placebo or active control-treated patients.

Conclusion

In spite of clear liver toxicity detected with a systematic surveillance program, liver safety signals were not identified from investigator adverse event reporting alone. By integrating key safety monitoring processes within the randomized design of adequately sized clinical trials, the rare but serious liver toxicity signal became clear, leading to timely program termination.

Keywords

Data monitoring committee fasiglifam hepatotoxicity

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References

Lewis

JH.

The art and science of diagnosing and managing drug-induced liver injury in 2015 and beyond. Clin Gastroenterol Hepatol 2015; 13(12): 2173.e8–2189.e8.

Zimmerman

HJ.

Hepatotoxicity: the adverse effects of drugs and other chemicals on the liver. 2nd ed. Philadelphia, PA: Lippincott Williams & Wilkins, 1999.

de Abajo

Montero

Madurga

et al . Acute and clinically relevant drug-induced liver injury: a population based case-control study. Br J Clin Pharmacol 2004; 58(1): 71–80.

Sgro

Clinard

Ouazir

et al . Incidence of drug-induced hepatic injuries: a French population-based study. Hepatology 2002; 36(2): 451–455.

Navarro

Senior

JR.

Drug-related hepatotoxicity. N Engl J Med 2006; 354: 731–739.

Janssen Pharmaceuticals Inc. Xarelto, https://www.xarelto.com/en/resources/major-studies (accessed 10 July 2017).

Negoro

Sasaki

Mikami

et al . Discovery of TAK-875: a potent, selective, and orally bioavailable GPR40 agonist. ACS Med Chem Lett 2010; 1(6): 290–294.

Naik

Vakilynejad

et al . Safety, tolerability, pharmacokinetics, and pharmacodynamic properties of the GPR40 agonist TAK-875: results from a double-blind, placebo-controlled single oral dose rising study in healthy volunteers. J Clin Pharmacol 2012; 52(7): 1007–1016.

Leifke

Naik

et al . A multiple-ascending-dose study to evaluate safety, pharmacokinetics, and pharmacodynamics of a novel GPR40 agonist, TAK-875, in subjects with type 2 diabetes. Clin Pharmacol Ther 2012; 92(1): 29–39.

10.

Takeda press release, December 2013, https://takedaclinicaltrials.com (Accessed 5th March 2019).

11.

Rockey

Seeff

Rochon

et al . Causality assessment in drug-induced liver injury using a structured expert opinion process: comparison to the Roussel-Uclaf causality assessment method. Hepatology 2010; 51(6): 2117–2126.

12.

Zimmerman

HJ.

The spectrum of hepatotoxicity. Perspect Biol Med 1968; 12: 135–161.

13.

Sumaya

Wallentin

James

et al . Fibrin clot properties independently predict adverse clinical outcome following acute coronary syndrome: a PLATO substudy. Eur Heart J 2018; 39(13): 1078–1085.

14.

Senior

JR.

Evolution of the Food and Drug Administration approach to liver safety assessment for new drugs: current status and challenges. Drug Saf 2014; 37(Suppl. 1): S9–S17.

15.

Watkins

Desai

Berkowitz

et al . Evaluation of drug-induced serious hepatotoxicity (eDISH): application of this data organization approach to phase III clinical trials of rivaroxaban after total hip or knee replacement surgery. Drug Saf 2011; 34: 243–252.

16.

Friedman

Furberg

DeMets

et al . Fundamentals of Clinical Trials. 5th ed. New York: Springer, 2015.

17.

Eypasch

Lefering

Kum

et al . Probability of adverse events that have not yet occurred: a statistical reminder. BMJ 1995; 311: 619–620.

18.

Keisu

Andersson

TB.

Drug-induced liver injury in humans: the case of ximelagatran. Handb Exp Pharmacol 2010; 196: 407–418.

19.

Lazerow

Abdi

Lewis

JH.

Drug-induced liver disease 2004. Curr Opin Gastroenterol 2005; 21: 283–292.

20.

Russmann

Niedrig

Budmiger

et al . Rivaroxaban postmarketing risk of liver injury. J Hepatol 2014; 61(2): 293–300.

21.

Hornby

StarkeyLewis

Dear

et al . MicroRNAs as potential circulating biomarkers of drug-induced liver injury: key current and future issues for translation to humans. Expert Rev Clin Pharmacol 2014; 7(3): 349–362.

22.

Osaki

Kosaka

Okada

et al . Circulating microRNAs in drug safety assessment for hepatic and cardiovascular toxicity: the latest biomarker frontier. Mol Diagn Ther 2014; 18(2): 121–126.

23.

Cowie

Blomster

Curtis

et al . Electronic health records to facilitate clinical research. Clin Res Cardiol 2017; 106(1): 1–9.

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