Severe acute pain occurs through nociceptive signalling involving both ascending and descending spinal pathways, in which nerve conductance is mediated in part by the action of opioid receptors. Opioid receptors are seven-transmembrane G-protein-coupled receptors (GPCRs), of which the μ-opioid receptor subtype is predominantly targeted by and is responsible for the effects of opioid agonists. However, due to the ability of some opioid agonists to bind to other targets, as well as activation of additional downstream pathways from opioid receptors such as those involving β-arrestin, the beneficial analgesic effects of opioids are coupled with severe adverse effects such as constipation and respiratory depression.
Oliceridine (formerly known as TRV130) is a "biased agonist" at the μ-opioid receptor by preferentially activating the G-protein pathway with minimal receptor phosphorylation and recruitment of β-arrestin. By acting as a biased agonist, oliceridine provides comparable analgesia compared with traditional opioids such as morphine at a comparable or decreased risk of opioid-related adverse effects such as constipation and respiratory depression.
Oliceridine was first reported in 2013, but was initially not approved by the FDA due to concerns raised by the Anesthetic and Analgesic Drug Products Advisory Committee. Oliceridine gained FDA approval on August 7, 2020, and is currently marketed by Trevena Inc as OLINVYK™.
用于成人治疗严重到需要静脉注射阿片类镇痛药的急性疼痛,并且替代治疗方法不足。
241 Huaihai West Road, Xuhui District, Shanghai, Shanghai, Shanghai, China
Dong-Xin Wang, Beijing, China
Regional One Health, Memphis, Tennessee, United States
Cleveland Clinic Fairview Hospital, Cleveland, Ohio, United States
Wake Forest Bapist Medical Center, Winston-Salem, North Carolina, United States
Cleveland Clinic Main Campus, Cleveland, Ohio, United States
Research Site, San Antonio, Texas, United States
Research Site, San Antonio, Texas, United States
Resarch Site, Salt Lake City, Utah, United States
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