Cebranopadol: novel dual opioid/NOP receptor agonist analgesic

Raffa, Robert B.; Burdge, G.; Gambrah, J.; Kinecki, H. E.; Lin, Fang-Tsyr; Lu, Biao; Nguyen, Julia; Phan, Vy; Ruan, A.; Sesay, Muctarr; Watkins, Tonya

doi:10.1111/jcpt.12461

Cited by 36 publications

(30 citation statements)

References 104 publications

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“…Morphine PR was selected as the active comparator in this trial given that it is well accepted that oral morphine is as effective as other oral opioids, and there is no conclusive evidence that other strong opioids are superior in efficacy to morphine (Caraceni et al, 2012;Wiffen et al, 2016). In addition, given that cebranopadol besides NOP receptor agonism also acts on opioid receptors Raffa et al, 2017;Schunk et al, 2014), a comparison of its effects to pure MOP agonism was appropriate as well. The use of rescue medication (morphine IR) was selected as a primary endpoint in this trial, assuming that the used amounts of medication would reflect the efficacy of the IMP in the management of cancer pain.…”

Section: Discussionmentioning

confidence: 99%

“…Cebranopadol is a novel, first‐in‐class, strong small‐molecule analgesic, characterized by a high nociceptin/orphanin FQ peptide (NOP) receptor (encoded by the opioid receptor‐like 1 [OPRL1] gene) (Mollereau et al., ) and opioid receptor agonistic activity (Linz et al., ; Raffa et al., ; Schunk et al., ). As NOP and opioid receptor agonists modulate pain via distinct yet related targets, targeting both mechanisms may be particularly suited to provide potent analgesia and a better tolerability profile than classical opioids (Linz et al., ).…”

Section: Introductionmentioning

confidence: 99%

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Cancer‐related chronic pain: Investigation of the novel analgesic drug candidate cebranopadol in a randomized, double‐blind, noninferiority trial

Eerdekens

Kapanadze

Koch

et al. 2019

European Journal of Pain

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Background Cancer‐related pain is a growing health problem given the increasing life expectancy of cancer patients. Opioids are commonly used to treat cancer‐related pain, but carry the risk of severe side effects, limiting their use. Cebranopadol is a first‐in‐class drug candidate, combining nociceptin/orphanin FQ peptide and opioid peptide receptor agonism. This trial examined the analgesic efficacy of cebranopadol compared with morphine prolonged release (PR) in patients with moderate‐to‐severe cancer‐related pain. Methods This double‐blind, parallel‐group, multiple‐dose trial was designed as noninferiority trial for efficacy of cebranopadol versus morphine PR. Planned with 524 patients, finally 126 patients were treated for up to 7 weeks (low accrual). The primary efficacy endpoint was the average amount of daily rescue medication intake (morphine immediate release) over the last 2 weeks of treatment. Results For the primary endpoint, noninferiority of cebranopadol with and superiority over morphine PR were demonstrated (Full Analysis Set: ∆[95%CI] = −7.48 mg [−12.05, −2.92]; Per Protocol Set: ∆[95%CI] = −4.67 mg [−9.25, −0.10]). The vast majority of patients (≥75%, either treatment) had clinically relevant pain reduction, and noninferiority on this secondary endpoint was not shown. Mostly used doses were ≤800 μg cebranopadol or ≤120 mg morphine PR daily. A total of 83.1% of patients on cebranopadol and 82.0% on morphine PR experienced treatment‐emergent adverse events. Conclusions Cebranopadol was effective, safe and well tolerated in the dose range tested (200–1,000 μg) in patients suffering from chronic moderate‐to‐severe cancer‐related pain and was superior to morphine PR on the primary endpoint. Significance Cebranopadol presents a new approach to treat cancer pain. The drug candidate was easy to titrate, safe and well tolerated, and as effective as morphine PR in patients suffering from chronic moderate‐to‐severe cancer‐related pain

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Cancer‐related chronic pain: Investigation of the novel analgesic drug candidate cebranopadol in a randomized, double‐blind, noninferiority trial

Eerdekens

Kapanadze

Koch

et al. 2019

European Journal of Pain

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“…This drug has long‐term analgesic effects in acute and chronic pain models, and its side effects are less severe than those of standard opioid drugs. Indeed, motor coordination and respiratory function remains unaltered at high doses, and tolerance is delayed compared with morphine (Sukhtankar et al, ; Linz et al, ; Schunk et al, ; Raffa et al, ). According to ClinicalTrials.gov (National Institutes of Health, ), seven Phase II clinical trials have been completed with cebranopadol.…”

Section: Clinical Interest Of the Multitarget Approachmentioning

confidence: 99%

Usefulness of knockout mice to clarify the role of the opioid system in chronic pain

Maldonado

Baños

2018

British J Pharmacology

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“…Cebranopadol is a novel new agent that combines dual, full agonist action at ORs and NOP receptors (53). It has demonstrated good efficacy and safety in a variety of preclinical models of acute pain and particularly potent efficacy in preclinical models of neuropathic pain (44).…”

Section: Dual Action On Nop and -Ormentioning

confidence: 99%

Toward an effective peripheral visceral analgesic: responding to the national opioid crisis

Camilleri

2018

American Journal of Physiology-Gastrointestinal and Liver Physi

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This minireiew summarizes recent new developments in visceral analgesics. This promising field is important, as a new approach to address abdominal pain with peripheral visceral analgesics is considered a key approach to addressing the current opioid crisis. Some of the novel compounds address peripheral pain mechanisms through modulation of opioid receptors via biased ligands, nociceptin/orphanin FQ opioid peptide (NOP) receptor, or dual action on NOP and μ-opioid receptor, buprenorphine and morphiceptin analogs. Other compounds target nonopioid mechanisms, including cannabinoid (CB2), N-methyl-d-aspartate, calcitonin gene-related peptide, estrogen, and adenosine A receptors and transient receptor potential (TRP) channels (TRPV1, TRPV4, and TRPM8). Although current evidence is based predominantly on animal models of visceral pain, early human studies also support the evidence from the basic and animal research. This augurs well for the development of nonaddictive, visceral analgesics for treatment of chronic abdominal pain, an unmet clinical need.

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Cebranopadol: novel dual opioid/NOP receptor agonist analgesic

Cited by 36 publications

References 104 publications

Cancer‐related chronic pain: Investigation of the novel analgesic drug candidate cebranopadol in a randomized, double‐blind, noninferiority trial

Cancer‐related chronic pain: Investigation of the novel analgesic drug candidate cebranopadol in a randomized, double‐blind, noninferiority trial

Usefulness of knockout mice to clarify the role of the opioid system in chronic pain

Toward an effective peripheral visceral analgesic: responding to the national opioid crisis

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