The duration of sleep promoting efficacy by dual orexin receptor antagonists is dependent upon receptor occupancy threshold

Gotter, Anthony L.; Winrow, Christopher J.; Brunner, John; Garson, Susan L.; Fox, Steven V.; Binns, Jacquelyn; Harrell, C. Meacham; Cui, Donghui; Yee, Ka Lai; Stiteler, Mark; Stevens, Joanne; Savitz, Alan T.; Tannenbaum, Pamela L.; Tye, Spencer J.; McDonald, Terrence; Yao, Lihang; Kuduk, Scott D.; Uslaner, Jason M.; Coleman, Paul J.; Renger, John J.

doi:10.1186/1471-2202-14-90

Cited by 84 publications

(93 citation statements)

References 40 publications

(72 reference statements)

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“…Circadian oscillations in orexin peptides A and B within cerebrospinal fluid correlate with arousal cycles12, and exogenous administration of the neuropeptides is sufficient to drive wakefulness in rodents, particularly during the inactive phase34. A lack of orexin signaling is associated with narcolepsy, a disorder characterized by uncontrollable sleep episodes and hypersomnolence5.…”

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confidence: 99%

Orexin 2 Receptor Antagonism is Sufficient to Promote NREM and REM Sleep from Mouse to Man

Gotter

Forman

Harrell

et al. 2016

Sci Rep

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Orexin neuropeptides regulate sleep/wake through orexin receptors (OX1R, OX2R); OX2R is the predominant mediator of arousal promotion. The potential for single OX2R antagonism to effectively promote sleep has yet to be demonstrated in humans. MK-1064 is an OX2R-single antagonist. Preclinically, MK-1064 promotes sleep and increases both rapid eye movement (REM) and non-REM (NREM) sleep in rats at OX2R occupancies higher than the range observed for dual orexin receptor antagonists. Similar to dual antagonists, MK-1064 increases NREM and REM sleep in dogs without inducing cataplexy. Two Phase I studies in healthy human subjects evaluated safety, tolerability, pharmacokinetics and sleep-promoting effects of MK-1064, and demonstrated dose-dependent increases in subjective somnolence (via Karolinska Sleepiness Scale and Visual Analogue Scale measures) and sleep (via polysomnography), including increased REM and NREM sleep. Thus, selective OX2R antagonism is sufficient to promote REM and NREM sleep across species, similarly to that seen with dual orexin receptor antagonism.

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confidence: 99%

Orexin 2 Receptor Antagonism is Sufficient to Promote NREM and REM Sleep from Mouse to Man

Gotter

Forman

Harrell

et al. 2016

Sci Rep

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“…This compound is a close structural analog of suvorexant, and the 30 mg/kg p.o. dose of DORA-12 being used here achieves a plasma Cmax of 2.02 μM with CSF exposure of 66 nM and ex vivo occupancy of 97%, and has been shown to promote sleep in rats (Gotter et al, 2013). …”

Section: Methodsmentioning

confidence: 99%

Hypothalamic orexin’s role in exacerbated cutaneous vasodilation responses to an anxiogenic stimulus in a surgical menopause model

Federici

Caliman

Molosh

et al. 2016

Psychoneuroendocrinology

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Distressing symptoms such as hot flashes and sleep disturbances affect over 70% of women approaching menopause for an average of 4–7 years, and recent large cohort studies have shown that anxiety and stress are strongly associated with more severe and persistent hot flashes and can induce hot flashes. Although high estrogen doses alleviate symptoms, extended use increases health risks, and current non-hormonal therapies are marginally better than placebo. The lack of effective non-hormonal treatments is largely due to the limited understanding of the mechanisms that underlie menopausal symptoms. One mechanistic pathway that has not been explored is the wake-promoting orexin neuropeptide system. Orexin is exclusively synthesized in the estrogen receptor rich perifornical hypothalamic region, and has an emerging role in anxiety and thermoregulation. In female rodents, estrogens tonically inhibit expression of orexin, and estrogen replacement normalizes severely elevated central orexin levels in postmenopausal women. Using an ovariectomy menopause model, we demonstrated that an anxiogenic compound elicited exacerbated hot flash-associated increases in tail skin temperature (TST, that is blocked with estrogen), and cellular responses in orexin neurons and efferent targets. Furthermore, systemic administration of centrally active, selective orexin 1 or 2 and dual receptor antagonists attenuated or blocked TST responses, respectively. This included the reformulated Suvorexant, which was recently FDA-approved for treating insomnia. Collectively, our data support the hypothesis that dramatic loss of estrogen tone during menopausal states leads to a hyperactive orexin system that contributes to symptoms such as anxiety, insomnia, and more severe hot flashes. Additionally, orexin receptor antagonists may represent a novel non-hormonal therapy for treating menopausal symptoms, with minimal side effects.

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“…Authier et al 2015JPTM 6/2/2016 A wide range of approved drugs are associated with drug induced sleep disturbances such as insomnia, including beta-blockers (Chang et al, 2013;Moser, 1979), corticosteroids (Ciriaco et al, 2013), selective serotonin-reuptake inhibitors (SSRI) (Asnis, et al, 1999) or acetylcholinesterase inhibitors (Cooke et al, 2006). Polysomnography is a well-established technique for sleep disturbance assessment and is well established in laboratory animal species commonly used for non-clinical drug SP testing including rodents (Gotter et al, 2013), dogs and non-human primates (Authier et al, 2014).…”

Section: Discussionmentioning

confidence: 99%

Safety Pharmacology Investigations on the Nervous System: An Industry Survey

Authier

2017

Journal of Pharmacological and Toxicological Methods

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Abstract:The Safety Pharmacology Society (SPS) conducted an industry survey in 2015 to identify industry practices as they relate to central, peripheral and autonomic nervous system ("CNS") drug safety testing. One hundred fifty-eight (158) participants from Asia (16%), Europe (20%) and North America (56%) responded to the survey. 52% of participants were from pharmaceutical companies (>1,000 employees). Oncology (67%) and neurology/psychiatry (66%) were the most frequent target indications pursued by companies followed by inflammation (48%), cardiovascular (43%), metabolic (39%), infectious (37%), orphan (32%) and respiratory (29%) diseases. Seizures (67% of participants), gait abnormalities (67%), tremors (65%), emesis (56%), sedation (52%) and salivation (47%) were the most commonly encountered CNS issues in pre-clinical drug development while headache (65%), emesis/nausea (60%), fatigue (51%) and dizziness (49%) were the most frequent issues encountered in Phase I clinical trials. 54% of respondents reported that a standard battery of tests applied to screen drug candidates was the approach most commonly used to address nonclinical CNS safety testing. A minority (14% of all participants) reported using electroencephalography (EEG) screening prior to animal inclusion on toxicology studies. The most frequent group size was n=8 for functional observation battery (FOB), polysomnography and seizure liability studies. FOB evaluations were conducted in a dedicated room (78%) by blinded personnel (66%) with control for circadian cycle (55%) effects (e.g., dosing at a standardized time; balancing time of day across treatment groups). The rat was reported as the most common species used for seizure liability, nerve conduction and drug-abuse liability testing.

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The duration of sleep promoting efficacy by dual orexin receptor antagonists is dependent upon receptor occupancy threshold

Cited by 84 publications

References 40 publications

Orexin 2 Receptor Antagonism is Sufficient to Promote NREM and REM Sleep from Mouse to Man

Orexin 2 Receptor Antagonism is Sufficient to Promote NREM and REM Sleep from Mouse to Man

Hypothalamic orexin’s role in exacerbated cutaneous vasodilation responses to an anxiogenic stimulus in a surgical menopause model

Safety Pharmacology Investigations on the Nervous System: An Industry Survey

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