Mechanistic Investigations Support Liver Safety of Ubrogepant

Smith, Brenda J.; Rowe, Josh; Watkins, Paul B.; Ashina, Messoud; Woodhead, Jeffrey L.; Sistare, Frank D.; Goadsby, PJ

doi:10.1093/toxsci/kfaa093

Cited by 15 publications

(17 citation statements)

References 38 publications

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“…MK‐3207, another gepant, was associated with delayed liver test abnormalities in phase I trials (ALT elevations following the discontinuation of MK‐3207 administration), which also led to discontinuation of its clinical development 23–25 . Integrated mechanistic data suggested that DILI associated with telcagepant and MK‐3207 was at least partly attributable to reactive metabolites 26 . In addition, it is believed that the formation of covalent adducts between MK‐3207 and endogenous liver proteins, which does not occur with atogepant, caused the delayed DILI.…”

Section: Discussionmentioning

confidence: 99%

“…[23][24][25] Integrated mechanistic data suggested that DILI associated with telcagepant and MK-3207 was at least partly attributable to reactive metabolites. 26 In addition, it is believed that the formation of covalent adducts between MK-3207 and endogenous liver proteins, which does not occur with atogepant, caused the delayed DILI. Atogepant is chemically distinct from telcagepant and MK-3207, and has characteristics hypothesized to be important for reducing the potential for DILI, such as greater potency and higher target engagement and, therefore, a lower dosing needed for clinical efficacy, and a reduced potential to form reactive metabolites.…”

Section: Discussionmentioning

confidence: 99%

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Atogepant Is Not Associated With Clinically Meaningful Alanine Aminotransferase Elevations in Healthy Adults

Min

Kraft

Bondiskey

et al. 2020

Clinical Translational Sci

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Atogepant is a potent, selective, oral calcitonin gene–related peptide (CGRP) receptor antagonist in development for migraine prevention. The chemical structure of atogepant is distinct from previous CGRP receptor antagonists, which were associated with elevated serum alanine aminotransferase (ALT) in clinical trials. Here, we report the safety, tolerability, and pharmacokinetics (PKs) of a once‐daily supratherapeutic dose (170 mg) of atogepant for 28 days from a randomized, double‐blind, placebo‐controlled phase I trial in healthy participants. Overall safety, hepatic safety, and plasma PK parameters were evaluated. Thirty‐four participants aged 23–55 years enrolled; 28 (82.4%) completed the study in accordance with the protocol. Multiple doses of 170 mg atogepant for 28 consecutive days were generally well‐tolerated. All adverse events (AEs; reported in 87.0% of the atogepant group; 72.7%, placebo) were mild in severity except one serious AE of subarachnoid hemorrhage due to a bicycle accident and not considered related to treatment. There were two discontinuations due to AEs, both with atogepant, one considered possibly related to treatment. Over 28 days of treatment, no participant receiving atogepant had an ALT elevation above 1.5 × upper limit of normal. Change from baseline in serum ALT levels was not different between atogepant and placebo. Atogepant is rapidly absorbed (median time to maximum plasma concentration, ~ 2 hours) with an apparent terminal half‐life of ~ 11 hours, and no evidence of accumulation after once‐daily dosing. Overall, atogepant at a high oral dose is safe and well‐tolerated in healthy participants with no clinically meaningful elevations in ALT.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Atogepant Is Not Associated With Clinically Meaningful Alanine Aminotransferase Elevations in Healthy Adults

Min

Kraft

Bondiskey

et al. 2020

Clinical Translational Sci

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“…Notably, the software was able to predict the safety profile for three potential migraine drug candidates. DILIsym successfully modeled the liver toxicity profiles of telcagepant and MK3207 and was also able to show the lower potential for hepatotoxicity with ubrogepant, an alternative migraine drug [63]. This ability to predict liver injury in drug development and also provide a better understanding of the mechanisms of DILI offers unique opportunities and promises in the hepatotoxicity field (Table 2).…”

Section: Quantitative Systems Pharmacology and Dilimentioning

confidence: 98%

“…While it was initially designed for one-time emergency contraception use, it has been approved for use for 3 months at a time for the treatment of uterine fibroids [71][72][73]. Several recent reports of Table 2 DILIsym predictions for telcagepant, MK-3207, and ubrogepant in a simulated patient population of healthy volunteers [63] ALT alanine aminotransferase, BID twice daily, N/A not applicable, q2h every 2 hours, QD once daily, ULN upper limit of normal hepatotoxicity associated with longer term use in fibroid treatment were found. For example, Meunier et al described a 58-year-old woman who developed fatigue, nausea, and abdominal discomfort followed by rising ALT/AST and international normalized ratio 2 months after beginning treatment with ulipristal acetate for symptomatic fibroids [74].…”

Section: Quantitative Systems Pharmacology and Dilimentioning

confidence: 99%

Drug-Induced Liver Injury: Highlights and Controversies in the Recent Literature

et al. 2021

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Drug-induced liver injury (DILI) remains an important, yet challenging diagnosis for physicians. Each year, additional drugs are implicated in DILI and this year was no different, with more than 1400 articles published on the subject. This review examines some of the most significant highlights and controversies in DILI-related research over the past year and their implications for clinical practice. Several new drugs were approved by the US Food and Drug Administration including a number of drugs implicated in causing DILI, particularly among the chemotherapeutic classes. The COVID-19 pandemic was also a major focus of attention in 2020 and we discuss some of the notable aspects of COVID-19-related liver injury and its implications for diagnosing DILI. Updates in diagnostic and causality assessments related to DILI such as the Roussel Uclaf Causality Assessment Method are included, mindful that there is still no single biomarker or diagnostic tool to unequivocally diagnose DILI. Glutamate dehydrogenase received renewed attention as being more specific than alanine aminotransferase. There were a few new reports of previously unrecognized hepatotoxins, including immune modulators and novel gene therapy drugs that we highlight. Updates and new developments of previously described hepatotoxins, such as immune checkpoint inhibitors and anti-tuberculosis drugs are reviewed. Finally, novel technologies such as organoid culture systems to better predict DILI preclinically may be coming of age and determinants of hepatocyte loss, such as calculating P ALT are poised to improve our current means of estimating DILI severity and the risk of acute liver failure.

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“…36 Recent studies on mechanistic investigations in both in vitro and in vivo models support liver safety of ubrogepant and reported that it has lower potential to cause hepatotoxicity than has been observed with telcagepant and MK-3207. 35,37,38 It has also been reported that ubrogepant use is not associated medication overuse headache. 31,33…”

Section: Ubrogepant (Mk-1602)mentioning

confidence: 98%

Gepants, calcitonin gene-related peptide antagonists, for abortive treatment of migraine: current status

Gaddam

Padi

2021

Int J Basic Clin Pharmacol

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Migraine is a neurovascular disorder characterized by unilateral, recurrent, pulsating, throbbing, and moderate to severe headache. Triptans use is often limited by their poor efficacy, reports of poor responders, and contraindicated in patients with cardiovascular disorders. Calcitonin gene-related peptide (CGRP), a neuropeptide, regulates vascular tonicity as well as potent pain mediator, and both the mechanisms involved in development of migraine headache. Gepants are non-peptide, small molecules, highly selective, and potent CGRP antagonists. These novel drugs have been approved for abortive treatment of acute migraine with or without aura. These are being evaluated for their effectiveness and showing promising results in the prevention of migraine. Gepants do not have vasoconstrictive properties, are safe to use in patients with cardiovascular risk, and best alternative to triptan therapy. These are available in tablet, orally disintegrating tablet, and nasal forms to improve patient compliance. Ubrogepant and rimegepant are the two oral CGRP antagonists approved whereas atogepant and zavegepant are at late stage of development for approval.

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Mechanistic Investigations Support Liver Safety of Ubrogepant

Cited by 15 publications

References 38 publications

Atogepant Is Not Associated With Clinically Meaningful Alanine Aminotransferase Elevations in Healthy Adults

Atogepant Is Not Associated With Clinically Meaningful Alanine Aminotransferase Elevations in Healthy Adults

Drug-Induced Liver Injury: Highlights and Controversies in the Recent Literature

Gepants, calcitonin gene-related peptide antagonists, for abortive treatment of migraine: current status

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