A Dose-Blind Extension Study With Double-blind, Placebo-Controlled, Randomized Withdrawal Period to Evaluate the Safety and Explore the Pharmacokinetics and Pharmacodynamics of TAK-994 in Adults With Narcolepsy With Cataplexy (Narcolepsy Type 1)

Adults with narcolepsy who have completed the TAK-994-1501 study will be able to take part in this study.
The main aim of this study is to check if participants have side effects from TAK-994.
Participants will take one of 3 different TAK-994 dose for 8 weeks.
Then, half the participants will continue with their dose of TAK-994 and half will take a placebo. In this study, a placebo will look like a TAK-994 tablet but will not have any medicine in it. Participants will take TAK-994 or placebo for 4 weeks.
Participants will visit the clinic for a final check-up 2 weeks after their last dose of TAK-994 or placebo.
The study doctors will check for side effects from TAK-994 and placebo throughout the study.
Participants will continue to record any narcolepsy symptoms as they did in Part B of the TAK 994-1501 study.

开始日期2021-04-30

申办/合作机构

Takeda Pharmaceutical Co., Ltd.

NCT04833049

/ Completed临床1期

A Phase 1 Study to Assess Absolute Bioavailability of TAK-994 and to Characterize Mass Balance, Pharmacokinetics, Absorption, Metabolism, and Excretion of [14C]TAK-994 in Male Healthy Subjects

The aim of this study is to understand how TAK-994 is processed by the body.
This study will require participants to stay at the clinical research unit for 3 weeks to be monitored after receiving TAK-994.

开始日期2021-04-14

申办/合作机构

Takeda Pharmaceutical Co., Ltd.

NCT04745767

/ Completed临床1期

A Phase 1, Open-Label, Randomized, Crossover Study to Evaluate the Relative Bioavailability of Different TAK-994 Formulations and the Effect of Food on These Formulations in Healthy Adult Subjects

It is hoped that TAK-994 will eventually help people with a sleep condition called narcolepsy. Narcolepsy is a condition that causes extreme sleepiness during the day, including falling asleep suddenly. Before then, the sponsor needs to understand how the body processes TAK-994.
The main aims of the study are to learn how the body processes 4 different new forms of TAK-994, when taken with food and without food, compared to a standard form of TAK-994.
At the first visit, the study doctor will check who can take part. Then the participants will be picked for 1 of 3 groups by chance. These groups of participants will take different new forms of TAK-994 and the standard form. They will take these with and without food. This will happen again 3 or 4 times but will take TAK-994 in a different order each time. After each treatment with TAK-994, the study doctors will check the amount of TAK-994 in the blood of the participants, over time. The study doctors will also check if the participants have any side effects from TAK-994.
Participants will wait 5 or more days between each dose to allow time for TAK-994 to completely leave their bodies. Participants will stay in the clinic during their treatment with TAK-994. They will stay in the clinic for 15 days or longer. Participants who have 4 treatments with TAK-994 will stay in the clinic for 20 days or longer.
Then, the clinic will telephone the participants 12 days after their final treatment of TAK-994 to check if they have any health problems.

开始日期2021-02-16

申办/合作机构

Takeda Pharmaceutical Co., Ltd.

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2025-04-01·TOXICOLOGICAL SCIENCES

TAK-994 mechanistic investigation into drug-induced liver injury

Article

作者: Zhu, Andy Z X ; Miyamoto, Kazumasa ; von Grotthuss, Marcin ; Kadali, Harisha ; Cebers, Gvido ; Tohyama, Kimio ; Dragan, Yvonne ; Wagoner, Matthew P ; von Hehn, Christian ; Yukawa, Tomoya ; Baker, Kevin S ; Uetrecht, Jack ; Faber, Samantha C ; Flores, Ramon ; Shinozawa, Tadahiro ; Sudo, Yusuke ; Diogo, Dorothée ; Smith, Erin N

Abstract:

The frequency of drug-induced liver injury (DILI) in clinical trials remains a challenge for drug developers despite advances in human hepatotoxicity models and improvements in reducing liver-related attrition in preclinical species. TAK-994, an oral orexin receptor 2 agonist, was withdrawn from phase II clinical trials due to the appearance of severe DILI. Here, we investigate the likely mechanism of TAK-994 DILI in hepatic cell culture systems examined cytotoxicity, mitochondrial toxicity, impact on drug transporter proteins, and covalent binding. Hepatic liabilities were absent in rat and nonhuman primate safety studies, however, murine studies initiated during clinical trials revealed hepatic single-cell necrosis following cytochrome P450 induction at clinically relevant doses. Hepatic cell culture experiments uncovered wide margins to known mechanisms of intrinsic DILI, including cytotoxicity (>100× Cmax/IC50), mitochondrial toxicity (>100× Cmax/IC50), and bile salt efflux pump inhibition (>20× Css, avg/IC50). A potential covalent binding liability was uncovered with TAK-994 following hepatic metabolism consistent with idiosyncratic DILI and the delayed-onset clinical toxicity. Although idiosyncratic DILI is challenging to detect preclinically, reductions in total daily dose and covalent binding can reduce the covalent body binding burden and, subsequently, the clinical incidence of idiosyncratic DILI.

2024-01-01·Pharmacology, biochemistry, and behavior

The orexin receptor 2 (OX2R)-selective agonist TAK-994 increases wakefulness without affecting cerebrospinal fluid orexin levels in cynomolgus monkeys

Article

作者: Yamada, Ryuji ; Narita, Naohiro ; Ishikawa, Takashi ; Kakehi, Masaaki ; Kimura, Haruhide

Orexin A (OX-A) and orexin B are neuropeptides produced in orexin neurons located in the lateral hypothalamus that exert multiple biological functions through the activation of orexin receptor 1 (OX1R) and orexin receptor 2 (OX2R) throughout the central nervous system. OX1R and OX2R have distinct functions: OX1R is involved in reward seeking, whereas OX2R has a pivotal role in sleep/wake regulation. OX2R-selective agonists are in development as novel therapeutic agents for the treatment of hypersomnia. However, their potential to induce orexin release, which may indirectly stimulate both OX1R and OX2R in vivo, is unclear. Herein, we assessed the effects of the OX2R-selective agonist TAK-994 on wakefulness and orexin release in monkeys. Oral administration of TAK-994 at 10 mg/kg in the beginning of the sleep phase (zeitgeber time [ZT] 12) significantly increased wakefulness time in monkeys but did not increase OX-A levels in monkey cisternal cerebrospinal fluid (CSF). Moreover, oral administration of TAK-994 (10 mg/kg) during the active phase (ZT1) did not increase OX-A levels in monkey CSF. These findings indicate that the OX2R agonist TAK-994 selectively activates OX2R in vivo and would not robustly induce spontaneous orexin release during the daytime or nighttime in monkeys.

2023-07-27·The New England journal of medicine1区 · 医学

Oral Orexin Receptor 2 Agonist in Narcolepsy Type 1

1区 · 医学

Article

作者: von Hehn, Christian ; Scammell, Thomas E ; Plazzi, Giuseppe ; Mignot, Emmanuel ; Wu, Jingtao ; Swick, Todd ; Du, Yeting ; Dauvilliers, Yves ; Meyer, Seetha ; Szakács, Zoltan ; Sheikh, Sarah I ; Inoue, Yuichi ; Del Río Villegas, Rafael ; Koundourakis, Elena ; Murthy, N Venkatesha ; Kadali, Harisha ; Rogers, Raquel ; von Rosenstiel, Philipp ; Hanson, Elizabeth ; Zeitz, Heidi

BACKGROUND:

Narcolepsy type 1 is caused by severe loss or lack of brain orexin neuropeptides.

METHODS:

We conducted a phase 2, randomized, placebo-controlled trial of TAK-994, an oral orexin receptor 2-selective agonist, in patients with narcolepsy type 1. Patients with confirmed narcolepsy type 1 according to clinical criteria were randomly assigned to receive twice-daily oral TAK-994 (30 mg, 90 mg, or 180 mg) or placebo. The primary end point was the mean change from baseline to week 8 in average sleep latency (the time it takes to fall asleep) on the Maintenance of Wakefulness Test (range, 0 to 40 minutes; normal ability to stay awake, ≥20 minutes). Secondary end points included the change in the Epworth Sleepiness Scale (ESS) score (range, 0 to 24, with higher scores indicating greater daytime sleepiness; normal, <10) and the weekly cataplexy rate.

RESULTS:

Of the 73 patients, 17 received TAK-994 at a dose of 30 mg twice daily, 20 received 90 mg twice daily, 19 received 180 mg twice daily, and 17 received placebo. The phase 2 trial and an extension trial were terminated early owing to hepatic adverse events. Primary end-point data were available for 41 patients (56%); the main reason for missing data was early trial termination. Least-squares mean changes to week 8 in average sleep latency on the MWT were 23.9 minutes in the 30-mg group, 27.4 minutes in the 90-mg group, 32.6 minutes in the 180-mg group, and -2.5 minutes in the placebo group (difference vs. placebo, 26.4 minutes in the 30-mg group, 29.9 minutes in the 90-mg group, and 35.0 minutes the 180-mg group; P<0.001 for all comparisons). Least-squares mean changes to week 8 in the ESS score were -12.2 in the 30-mg group, -13.5 in the 90-mg group, -15.1 in the 180-mg group, and -2.1 in the placebo group (difference vs. placebo, -10.1 in the 30-mg group, -11.4 in the 90-mg group, and -13.0 in the 180-mg group). Weekly incidences of cataplexy at week 8 were 0.27 in the 30-mg group, 1.14 in the 90-mg group, 0.88 in the 180-mg group, and 5.83 in the placebo group (rate ratio vs. placebo, 0.05 in the 30-mg group, 0.20 in the 90-mg group, and 0.15 in the 180-mg group). A total of 44 of 56 patients (79%) receiving TAK-994 had adverse events, most commonly urinary urgency or frequency. Clinically important elevations in liver-enzyme levels occurred in 5 patients, and drug-induced liver injury meeting Hy's law criteria occurred in 3 patients.

CONCLUSIONS:

In a phase 2 trial involving patients with narcolepsy type 1, an orexin receptor 2 agonist resulted in greater improvements on measures of sleepiness and cataplexy than placebo over a period of 8 weeks but was associated with hepatotoxic effects. (Funded by Takeda Development Center Americas; TAK-994-1501 and TAK-994-1504 ClinicalTrials.gov numbers, NCT04096560 and NCT04820842.).

项与 Firazorexton 相关的新闻（医药）

2024-09-10

·EndPoints

Centessa to take narcolepsy drug into Phase 2 after no sign of side effects that doomed earlier competitor

Centessa Pharmaceuticals plans to take its orexin receptor 2 agonist into mid-stage testing for narcolepsy after a Phase 1 study showed signs of efficacy. The drug, ORX750, was tested in sleep-deprived healthy volunteers and showed positive results in helping them stay awake. Importantly, the company said Tuesday that there were “no observations of frequently reported on-target adverse events” that have been associated with the drug class. The drug developer said it plans to start Phase 2 trials in the fourth quarter of this year in patients with narcolepsy type 1 and type 2, and also with idiopathic hypersomnia, a condition that’s marked by excessive sleeping and daytime sleepiness. Side effects associated with the class have included visual disturbances and liver toxicities. Those liver effects led to the halt of work on a Takeda drug, TAK-994, back in 2021 . But the Japanese drugmaker earlier this year announced its own positive efficacy data from a related molecule, TAK-861, and has said it plans to take it into Phase 3 as soon as possible. Alkermes also has a drug in Phase 2 testing. Editor’s note: This story contained an error describing the study’s endpoint and has been corrected.

临床2期临床结果临床1期临床失败

2024-02-09

·FierceBiotech

Takeda powers toward pivotal trials after phase 2b narcolepsy win but pauses multi-indication dream

Takeda plans to move TAK-861 into phase 3 in the first half of its 2024 financial year. Takeda’s narcolepsy work has finally yielded a phase 2b win, albeit with a blemish. After axing one asset over liver toxicity, the Japanese drugmaker’s continued faith in the mechanism has been rewarded with a primary endpoint hit—but the midphase program only supports progression in one form of the disease. The phase 2b program featured two trials, one in narcolepsy type 1 (NT1) and another in narcolepsy type 2 (NT2). Both studies tested TAK-861, an oral orexin receptor 2 agonist. The potential of the mechanism is clearer in NT1, a condition characterized by deficiency of the neuropeptide orexin, but Takeda saw an opportunity to move the needle in NT2, too. Orexin levels are normal in patients with NT2. Takeda’s bet on NT2, a rarer, normally milder form of narcolepsy, has failed to make the case for further development of TAK-861 in the indication. But the drugmaker is more encouraged by the results in NT1, leading it to outline plans to start phase 3 trials in that form of the condition this year. The NT1 clinical trial randomized 112 patients to receive one of four oral doses of TAK-861 or placebo. After eight weeks, Takeda saw “statistically significant and clinically meaningful improvement in objective and subjective measures of wakefulness compared to placebo.” The measures included the maintenance of wakefulness test, the primary endpoint. Takeda hit the endpoint with a p-value of less than 0.001. An earlier trial of TAK-994, another oral orexin receptor 2 agonist, suggested the mechanism could “take a type 1 narcolepsy patient and make them look like a healthy individual,” Andy Plump, M.D., Ph.D., the president of R&D at Takeda, told investors in July. Liver toxicity forced Takeda to dump that candidate, but it identified the more potent TAK-861 as a molecule that could better balance the benefits and risks. Takeda is yet to share full safety data from the TAK-861 studies but said the treatment was generally safe and well tolerated in both trials, with no treatment-related serious adverse events, hepatotoxicity cases or visual disturbances. Buoyed by the data, Takeda plans to move into phase 3 in the first half of its 2024 financial year, which starts in April. The timing keeps Takeda tucked in behind NLS Pharmaceutics, which planned to start a phase 3 trial last month, in the race to bring an orexin 2 receptor agonist to market in NT1. Another rival, Jazz Pharmaceuticals, paused a phase 1 trial last year over visual disturbances and cardiovascular effects. Takeda retains an interest in NT2 and other conditions with normal levels of orexin. The company is still analyzing its data to inform the next steps in those settings and is “progressing multiple orexin agonists.” Plump previously laid out several paths that Takeda could take after seeing the phase 2b data, noting the potential to advance in NT1, NT1 plus NT2 or both settings plus additional indications.

临床2期临床失败

2024-02-09

·Firstwordpharma

Phase IIb success propels Takeda's narcolepsy asset into late-stage testing

Takeda announced plans to initiate Phase III studies for its oral orexin receptor 2 (OX2R) agonist TAK-861 in narcolepsy type 1 (NT1), following positive findings from a Phase IIb trial. Sarah Sheikh, head of global development, said the “clear and compelling results” enable the company to commence late-stage testing as early as the first half of fiscal year 2024. The Phase IIb study, involving 112 patients with NT1, demonstrated statistically significant and clinically meaningful improvements in both objective and subjective measures of wakefulness for TAK-861 versus placebo at week 8. The primary endpoint, a maintenance of wakefulness test, was consistent with key secondary outcome measures, including the Epworth Sleepiness Scale and Weekly Cataplexy Rate. The drug was well tolerated, with no treatment-related serious adverse events.Takeda, which also ran a Phase IIb trial of TAK-861 in narcolepsy type 2 (NT2), stated it had no intentions of advancing the candidate in this indication. Findings from both studies will be presented at an upcoming scientific conference.Not all rosesTakeda’s orexin franchise encountered troubled waters in late 2021, when the Phase II programme for another oral OX2R agonist TAK-994 in NT1 and NT2 was axed after the emergence of a safety signal. The franchise also includes an investigational intravenous OX2R agonist TAK-925.Sheikh remarked that the drugmaker will continue to leverage its “deep and growing understanding of orexin biology” to investigate multiple orexin agonists across a wide range of indications, including conditions with normal orexin levels such as NT2.

临床2期临床结果临床失败

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适应症	最高研发状态	国家/地区	公司	日期
猝倒症	临床2期	美国	Spera Pharma, Inc.	2020-02-28
猝倒症	临床2期	加拿大	Spera Pharma, Inc.	2020-02-28
猝倒症	临床2期	捷克	Spera Pharma, Inc.	2020-02-28
猝倒症	临床2期	芬兰	Spera Pharma, Inc.	2020-02-28
猝倒症	临床2期	法国	Spera Pharma, Inc.	2020-02-28
猝倒症	临床2期	匈牙利	Spera Pharma, Inc.	2020-02-28
猝倒症	临床2期	意大利	Spera Pharma, Inc.	2020-02-28
猝倒症	临床2期	荷兰	Spera Pharma, Inc.	2020-02-28
猝倒症	临床2期	西班牙	Spera Pharma, Inc.	2020-02-28
发作性睡病	临床2期	荷兰	武田（中国）国际贸易有限公司	2020-02-28

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研究	分期	人群特征	评价人数	分组	结果	评价	发布日期


NCT04096560 (CTgov)	临床2期	猝倒症	97	Placebo (Part A: Placebo)	繭鑰夢淵膚醖醖餘窪淵 = 齋鏇廠襯衊餘顧網窪衊淵願鑰鏇淵顧憲壓獵簾 (餘襯糧選醖願鹹製醖膚, 繭衊蓋壓壓淵積餘鏇艱 ~ 醖願築鬱醖簾繭醖淵艱) 更多	-	2024-10-29
				TAK-994 (Part A: TAK-994 120 mg)	繭鑰夢淵膚醖醖餘窪淵 = 獵顧膚窪顧憲夢鹽膚遞淵願鑰鏇淵顧憲壓獵簾 (餘襯糧選醖願鹹製醖膚, 鹹壓餘鑰膚網觸糧襯醖 ~ 夢襯艱糧選獵淵餘遞憲) 更多
WSC2023	N/A	睡眠剥夺	-	TAK-994 high-dose (HD)	鬱艱範鹹襯簾簾膚獵醖(積構鬱觸齋衊繭窪壓衊) = Urinary-related events were the most frequently reported TEAEs with TAK-994 膚膚網選範憲鹽膚淵膚 (夢鏇壓網襯繭衊壓築蓋 )	-	2023-10-23
				TAK-994 low-dose (LD)
NCT04096560 \| NCT04820842 (Literature \| Pubmed \| N Engl J Med) 人工标引	临床2期	发作性睡病	73	TAK-994 30 mg	膚膚鏇衊製廠願窪壓顧(衊廠選窪顧築顧鬱繭範) = 艱鏇積鹹廠壓糧顧鏇艱憲願築鏇壓顧襯壓鑰鏇 (鹽顧鏇獵糧鏇蓋膚窪範 ) 更多	不佳	2023-07-27
				TAK-994 90 mg	膚膚鏇衊製廠願窪壓顧(衊廠選窪顧築顧鬱繭範) = 遞構鑰獵齋繭觸齋獵築憲願築鏇壓顧襯壓鑰鏇 (鹽顧鏇獵糧鏇蓋膚窪範 ) 更多