A Phase 2a, Randomized, Double-blind, Placebo-controlled Study of the Safety, Tolerability, Pharmacokinetics, and Pharmacodynamics of ORX750 in Subjects With Narcolepsy and Idiopathic Hypersomnia (CRYSTAL-1)

Narcolepsy Type 1 (NT1), Narcolepsy Type 2 (NT2), and Idiopathic Hypersomnia (IH) are rare conditions that make people feel very sleepy during the day (often referred to as excessive daytime sleepiness [EDS]). People living with these conditions might find it hard to stay alert and pay attention when they are at school, working, driving, or performing other daily activities.
While all conditions result in feeling sleepy, there are some differences in other common symptoms:
* NT1: People with NT1 often feel very tired during the day and experience cataplexy. Cataplexy is a sudden loss of muscle strength, which can cause someone to collapse or lose control of their muscles for a short time. This is often triggered by strong emotions, such as laughter or surprise. They may also have trouble sleeping well at night.
* NT2: People with NT2 feel sleepy during the day, just like NT1, but they do not have cataplexy.
* IH: People with IH feel tired during the day, even after sleeping a lot at night. They may sleep for long periods, take long naps, and find it hard to wake up.
Orexin is a protein in the brain that helps coordinate a system that plays an important role in helping people to stay awake during the daytime. Cleminorexton (also known as ORX750) is designed to mimic the action of orexin. The purpose of this study is to see how safe and tolerable ORX750 is in NT1, NT2, and IH, and learn about what the drug does to the body. Another goal of the study is to see if ORX750 can help people with NT1, NT2, and IH feel less sleepy and make other symptoms better.

Start Date23 Dec 2024

Sponsor / Collaborator

Centessa Pharmaceuticals Plc

100 Clinical Results associated with Cleminorexton

100 Translational Medicine associated with Cleminorexton

100 Patents (Medical) associated with Cleminorexton

Literatures (Medical) associated with Cleminorexton

01 Nov 2025·CURRENT OPINION IN PULMONARY MEDICINE

Understanding idiopathic hypersomnia: diagnosis, pathophysiology, and management

Review

Author: Renee Monderer ; Madeeha Shahzadi ; Michael J. Thorpy

Purpose of review:

Idiopathic hypersomnia is a chronic and often disabling sleep disorder characterized by excessive daytime sleepiness despite adequate or prolonged nighttime sleep. With recent advances in diagnosis and treatment, this review is timely in addressing evolving approaches to understanding and managing idiopathic hypersomnia, a condition that remains underrecognized and frequently misdiagnosed.

Recent findings:

Idiopathic hypersomnia is clinically distinct from narcolepsy, lacking REM-related features such as cataplexy and hypnagogic hallucinations. Until recently, treatment options for idiopathic hypersomnia were limited and often off-label. The 2021 FDA approval of low-sodium oxybate (LXB) marked the first medication specifically indicated for idiopathic hypersomnia. Additional agents such as modafinil, pitolisant, and traditional stimulants are used off-label with varying efficacy. Ongoing research is exploring promising treatments, including orexin-2 receptor agonists (e.g. ALKS 2680, ORX-750), serdexmethylphenidate, and flumazenil, which offer new hope for personalized management.

Summary:

Growing insights into the pathophysiology and clinical features of idiopathic hypersomnia have led to improved diagnostic clarity and therapeutic innovation. These developments carry significant implications for clinical practice, offering hope for better symptom control and quality of life in affected individuals. Ongoing research is crucial for refining treatment strategies and deepening our understanding of this complex condition.

01 Jun 2015·Journal of neural transmission (Vienna, Austria : 1996)Q4 · MEDICINE

Orexin excites rat inferior vestibular nuclear neurons via co-activation of OX1 and OX2 receptors

Q4 · MEDICINE

Article

Author: Zhuang, Qian-Xing ; Zhu, Jing-Ning ; Zhang, Xiao-Yang ; Yu, Lei ; Wang, Jian-Jun ; Chen, Zhang-Peng

Orexin deficiency results in cataplexy, a motor deficit characterized by sudden loss of muscle tone, strongly indicating an active role of central orexinergic system in motor control. However, effects of orexin on neurons in central motor structures are still largely unknown. Our previous studies have revealed that orexin excites neurons in the cerebellar nuclei and lateral vestibular nucleus, two important subcortical motor centers for control of muscle tone. Here, we report that both orexin-A and orexin-B depolarizes and increases the firing rate of neurons in the inferior vestibular nucleus (IVN), the largest nucleus in the vestibular nuclear complex and holding an important position in integration of information signals in the control of body posture. TTX does not block orexin-induced excitation on IVN neurons, suggesting a direct postsynaptic action of the neuropeptide. Furthermore, bath application of orexin induces an inward current on IVN neurons in a concentration-dependent manner. SB334867 and TCS-OX2-29, specific OX1 and OX2 receptor antagonists, blocked the excitatory effect of orexin, and [Ala(11), D-Leu(15)]-orexin B, a selective OX2 receptor agonist, mimics the orexin-induced inward current on IVN neurons. qPCR and immunofluorescence results show that both OX1 and OX2 receptor mRNAs and proteins are expressed and localized in the rat IVN. These results demonstrate that orexin excites the IVN neurons by co-activation of both OX1 and OX2 receptors, suggesting that via the direct modulation on the IVN, the central orexinergic system may actively participate in the central vestibular-mediated postural and motor control.

01 Mar 2007·Journal of physiology and pharmacology : an official journal of the Polish Physiological Society

Effects of somatostatin-14 and the receptor-specific somatostatin analogs on chromogranin A and alpha-subunit (alpha-SU) release from "clinically nonfunctioning" pituitary adenoma cells incubated in vitro.

Article

Author: Pawlikowski, M ; Radek, M ; Kunert-Radek, J ; Lawnicka, H ; Pisarek, H ; Culler, M D

The aim of the study was to examine the effect of somatostatin (SST) and its analogs on the release of chromogranin A (CgA) and alpha-subunit (alpha-SU) from clinically non-functioning pituitary adenomas incubated in vitro. Seven pituitary macroadenomas surgically removed were investigated. All of the tumors were diagnosed before surgery as non-functioning, but they expressed either gonadotropins or their subunits as detected by immunohistochemistry. Two tumors additionally expressed prolactin and growth hormone. All adenomas also expressed chromogranin A (CgA) and at least 3 of 5 subtypes of somatostatin receptors. The cells isolated from the examined tumors were exposed in vitro to either native SST-14 or the following receptor-specific SST analogs: BIM-23926 (agonist of sst1 receptor), BIM-23120 (agonist of sst2 receptor), BIM-23206 (agonist of sst5 receptor) and BIM23A387 (somatostatin/dopamine chimera). The concentration of CgA was measured by means of ELISA method and of alpha-SU was measured by an immunoradiometric method. It was found that the exposure on SST-14 resulted in the decrease of CgA and alpha-SU release from tumor cells in majority of samples, and the effect on CgA was positively correlated with the expression of sst3 and also with the sst2A/sst2B expressions ratio. The inhibitory effect of SST-14 on CgA and alpha-SU seems also to correlate negatively with the expression of sst2B. CgA inhibition also correlates positively with sst5 expression. Among the other compounds studied, only the sst2 agonist decreased the release in all the investigated samples. The remaining substances (agonists of sst1 and sst5 and SST/DA chimera) produced the divergent changes (increased or decreased release, depending on the sample). The data suggest that the inhibition of CgA (and possibly of alpha-SU) release by SST is mediated via subtypes sst2A, sst3 and sst5, whereas sst2B subtype may induce the opposite effect.

News (Medical) associated with Cleminorexton

10 Apr 2026

·pmlive.com

Lilly to acquire Centessa in deal worth up to $7.8bn

Eli Lilly (Lilly) has agreee to acquire Centessa Pharmaceuticals in a deal worth up to $7.8bn. Centessa is a clinical-stage company focused on developing treatments for excessive daytime sleepiness and other neurological conditions. Designed to treat narcolepsy and other sleep-wake disorders, Centessa is advancing a pipeline of orexin receptor 2 (OX2R) agonists. The company’s lead candidate, cleminorexton (formerly ORX750), demonstrated a potential best-in-class profile in phase 2a clinical studies across narcolepsy type 1, narcolepsy type 2 and idiopathic hypersomnia. Carole Ho, executive vice president and president of Lilly Neuroscience, said: “Orexin receptor biology represents one of the most compelling mechanistic opportunities in neuroscience as a direct intervention on the master switch of the sleep-wake cycle. “Centessa has assembled a portfolio with the breadth and depth to improve wakefulness across a broad array of indications.” Mario Alberto Accardi, CEO of Centessa and founder of the Orexin Program, said: “By combining Centessa’s team and capabilities with Lilly’s global complementary research, clinical, regulatory and commercial capabilities, we will seek to accelerate the advancement of our orexin portfolio across a broad range of neuroscience indications for the benefit of patients in need.” Both companies’ boards of directors have approved the transaction, which is expected to close in the third quarter of 2026.

Phase 2Acquisition

07 Apr 2026

·endpoints.news

Eli Lilly's latest acquisition could preview another booming market

Eli Lilly may not have discovered orexins, but the pharma’s latest acquisition marks increasing momentum for a drug class that’s maturing after years of fine-tuning. The big question on the minds of Wall Street is whether orexins’ potential is fully known. Lilly announced last week that it was buying Centessa Pharmaceuticals for $6.3 billion upfront, its largest acquisition since it bought Loxo Oncology in 2019, should the deal close. The move gives Lilly access to a pipeline of orexin receptor 2 agonists, primarily in development to treat sleep disorders like narcolepsy. But what if narcolepsy is just scratching the surface? Interviews with Wall Street analysts suggest that’s a possibility, and with Lilly in control, a lot more money could be poured into widening the drugs’ development scope — specifically, testing whether they broadly help with focus or fatigue. “It’s not a small, little number that they’re paying for this. And clearly Lilly believes there’s something here,” Leerink Partners senior managing director Marc Goodman said. Goodman laid out an all-too-familiar potential circumstance for those who closely watched the development of the diabetes and weight loss drugs. Novo Nordisk, a cardiometabolic powerhouse, was first to market with Ozempic, then Wegovy. But Lilly has since snagged a majority of the injectable market share, and with it a dominant position atop the largest current drug market and possibly the largest ever. Does history dare repeat itself? The orexin race is currently led by Takeda, which had its new drug application accepted by the FDA in February and is expecting a decision in the third quarter. Alkermes has a candidate in Phase 3, followed by Centessa in Phase 2. But those assets are focused on narcolepsy or idiopathic hypersomnia, a condition marked by excessive daytime sleepiness. “Now to me, all of a sudden, the Centessa asset, or I should say, the second asset, and the third asset … I think those are strategically advantaged versus the Alkermes ones big-time because of Lilly acquiring them,” Goodman said. Behind Centessa’s lead asset ORX750 are two others: Phase 1-stage ORX142, which is broadly aimed at neurodegenerative and neurological conditions; and ORX489 for neuropsychiatric conditions. The latter is still in preclinical development. Alkermes is shining a light on where these drugs might go next. Its two follow-up orexin candidates, both in the clinic, are aimed at neurodegenerative disease-related fatigue and attention deficit hyperactivity disorder. Paul Matteis, managing director and head of therapeutics research at the investment bank Stifel, said Lilly could ultimately end up being a tailwind for the whole class as more proof-of-concept data are generated across a host of additional conditions. “It’s going to increase the breadth of use for the whole class, even if there might be some molecules that are first here, first there,” Matteis told Endpoints News . The final pillar of the drug market that Lilly could capitalize on is how these drugs actually make it to patients. The Indianapolis pharma has been building its direct-to-consumer infrastructure on the back of its GLP-1 portfolio , and that may be a potential distribution stream for future orexin drugs. Matteis and Goodman both said it’s a worthwhile consideration, but that it would be unlikely to impact the sleep disorder market, given they expect the price of these drugs to cost hundreds of thousands of dollars. “I think that’s something that you could see with a next-generation drug, but I don’t think it would be with these first generations,” Matteis said.

AcquisitionPhase 2Phase 3

04 Apr 2026

·endpoints.news

Pharma’s dealmaking tear; Blackstone raises record fund; Xolair energizes allergy research; and more

Welcome back to Endpoints Weekly! They say March comes in like a lion and out like a lamb, but two pharma giants made a roar this week with megadeals worth more than $5 billion upfront. If the pharma industry keeps it up, it could outpace last year’s already-strong M&A figures. Our team also tracked developments this week on Eli Lilly’s obesity pill and President Donald Trump’s plans for pharmaceutical tariffs. You can read Anna Brown’s story here for the details on Trump’s executive order. — Nicole DeFeudis 🤝 Several pharma companies have inked deals in the last couple weeks, including two $5 billion-plus upfront deals that were disclosed on Tuesday morning alone. Here’s what you need to know: Eli Lilly said it would pay $6.3 billion upfront and up to $1.5 billion in contingent value rights to acquire Centessa Pharmaceuticals and its orexin receptor 2 agonists. It’s Lilly’s third acquisition of the year, but its largest since the $8 billion takeover of Loxo Oncology in 2019. Centessa’s lead drug, called cleminorexton (ORX750), is in Phase 2a testing for narcolepsy type 1, narcolepsy type 2 and idiopathic hypersomnia. That same day, Biogen unveiled a $5.6 billion deal to acquire Apellis Pharmaceuticals. The deal comes with two approved drugs, most notably a rare blood disorder drug called Empaveli, which was also approved last year for a rare kidney disease — and Biogen execs think this could be its next big market. Across March, biopharmas lined up 10 acquisitions worth up to $31.5 billion, according to an Endpoints tally. If the pace continues, 2026 could surpass 2025, which was already a standout year for M&A, Kyle LaHucik wrote in this analysis . Jon Norris, a healthcare banker at HSBC, told Endpoints that he thinks the M&A pace will remain, “though maybe not at the frenzy we saw in Q1.” 💰Blackstone this week announced it had raised $6.3 billion for its latest life sciences vehicle, Blackstone Life Sciences VI — the industry’s largest-ever private investment fund . It’s equal to more than half the value of new investment funds raised all of last year, according to a year-end report from William Blair. Blackstone has already deployed about $2 billion from the fund over the past 12 months, and could continue investing at a pace of about $1.5 billion to $2 billion a year, Nick Galakatos, global head of Blackstone Life Sciences, told Endpoints. The fund lands as the biotech industry pulls out of a yearslong slump , but Blackstone is also taking a different strategy than most. Instead of high-risk, early-stage bets, Blackstone tends to back late-stage development programs. Read more from Kyle LaHucik here . 🥜 The surge in food allergies transformed how many American children grow up. But a combination of better biological understanding, and a new use of an old drug, has cracked open a potentially huge market in biopharma — and effective treatments for patients. We took a comprehensive look at how Roche and Novartis’ Xolair, a 23-year-old asthma medicine, found renewed life as a blockbuster after it won expanded approval in 2024 to treat food allergies. Big pharma is ready to engage, too. GSK and Novartis both snapped up allergy biotechs this year. A crop of biotechs has also raised more than $240 million in the last 12 months (including the one Novartis acquired). The resurgence suggests a clear and eager demand among patients and families for new treatments. Read more from Max Gelman here . 💊A new competition is brewing, as Eli Lilly brings its obesity pill to market. The FDA announced on Wednesday that it approved orforglipron under its new Commissioner’s National Priority Voucher program. Lilly plans to market the pill as Foundayo, but as with the obesity shots Novo and Lilly have both brought to market, the Indianapolis drugmaker will be second to reach patients. Lilly suggested that Foundayo might have an edge over the Wegovy pill in its relative ease of use. It plans to start selling Foundayo on its direct-to-consumer platform LillyDirect, with shipping beginning April 6. Get more details here.

Drug ApprovalAcquisitionPhase 2

100 Deals associated with Cleminorexton

R&D Status

10 top R&D records.

to view more data

Indication	Highest Phase	Country/Location	Organization	Date
Idiopathic Hypersomnia	Phase 2	-	Centessa Pharmaceuticals Plc	13 Nov 2024
Narcolepsy	Phase 2	-	Centessa Pharmaceuticals Plc	13 Nov 2024

Clinical Result

Indication

Phase

Evaluation

View All Results

Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


AAN 12025 \| AAN 22025 Manual	Phase 1	Sleep Deprivation	-	ORX750 1.0 mg	ljklsmcgqp(cnyllrkoca) = quvrsozxet xesuzkegtm (fsgmotcacw, 12.1 - 23.2) View more	Positive	08 Apr 2025
				ORX750 2.5 mg	ljklsmcgqp(cnyllrkoca) = ashtikezln xesuzkegtm (fsgmotcacw, 22.2 - 41.8) View more
GlobeNewswire Manual	Phase 1	-	26	ORX750ORX750 1.0 mg	bfbjivnldu(lgafriucdc) = xcblzvmnte zatykffenz (eyrnsybjxd, 12 - 23)	Positive	12 Nov 2024
				ORX750ORX750 2.5 mg	bfbjivnldu(lgafriucdc) = ggcfcgjang zatykffenz (eyrnsybjxd, 22 - 42)
GlobeNewswire Manual	Phase 1	-	36	ORX750	fxvnbkqzva(cfypgcbzmc) = uoimyoopub ewimvzaqbn (hqjlwshghe )	Positive	10 Sep 2024
				Placebo	fxvnbkqzva(cfypgcbzmc) = egrlilcgiq ewimvzaqbn (hqjlwshghe )

Translational Medicine

Boost your research with our translational medicine data.

view full example data

Deal

Boost your decision using our deal data.

view full example data

Core Patent

Boost your research with our Core Patent data.

view full example data

Clinical Trial

Identify the latest clinical trials across global registries.

view full example data

Approval

Accelerate your research with the latest regulatory approval information.

view full example data

Regulation

Understand key drug designations in just a few clicks with Synapse.

view full example data

AI Agents Built for Biopharma Breakthroughs

Accelerate discovery. Empower decisions. Transform outcomes.

Get started for free today!

Accelerate Strategic R&D decision making with Synapse, PatSnap’s AI-powered Connected Innovation Intelligence Platform Built for Life Sciences Professionals.

Start your data trial now!

Synapse data is also accessible to external entities via APIs or data packages. Empower better decisions with the latest in pharmaceutical intelligence.

Bio

Bio Sequences Search & Analysis

Chemical

Chemical Structures Search & Analysis

Cleminorexton

Overview

Basic Info

Related

R&D Status

Clinical Result

Translational Medicine

Deal

Core Patent

Clinical Trial

Approval

Regulation