| Literature DB >> 33115393 |
Kanako Miyano1, Sei Manabe1, Akane Komatsu1, Yuriko Fujii1, Yusuke Mizobuchi1, Eiko Uezono1, Kaori Ohshima1, Miki Nonaka1, Yui Kuroda2, Minoru Narita1, Yasuhito Uezono1.
Abstract
Opioid agonists elicit their analgesic action mainly via μ opioid receptors; however, their use is limited because of adverse events including constipation and respiratory depression. It has been shown that analgesic action is transduced by the G protein-mediated pathway whereas adverse events are by the β-arrestin-mediated pathway through μ opioid receptor signaling. The first new-generation opioid TRV130, which preferentially activates G protein- but not β-arrestin-mediated signal, was constructed and developed to reduce adverse events. TRV130 and other G protein-biased compounds tend to elicit desirable analgesic action with less adverse effects. In clinical trials, the intravenous TRV130 (oliceridine) was evaluated in Phase I, II and III clinical studies. Here we review the discovery and synthesis of TRV130, its main action as a novel analgesic having less adverse events, its up-to-date status in clinical trials, and additional concerns about TRV130 as demonstrated in the literature. Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.Entities:
Keywords: Adverse β-arrestin effects; Agonists; Biased ligands; Oliceridine; TRV130; μ Opioid receptors
Mesh:
Substances:
Year: 2020 PMID: 33115393 DOI: 10.2174/1568026620999201027224229
Source DB: PubMed Journal: Curr Top Med Chem ISSN: 1568-0266 Impact factor: 3.295