Novel N-Substituted Benzomorphan-Based Compounds: From MOR-Agonist/DOR-Antagonist to Biased/Unbiased MOR Agonists

Lorella Pasquinucci,Carmela Parenti,M. Carmen Ruiz-Cantero,Zafiroula Georgoussi,Paschalina Pallaki,Enrique J. Cobos,Emanuele Amata,Agostino Marrazzo,Orazio Prezzavento,Emanuela Arena,Maria Dichiara,Loredana Salerno,Rita Turnaturi

Novel N-Substituted Benzomorphan-Based Compounds: From MOR-Agonist/DOR-Antagonist to Biased/Unbiased MOR Agonists

2020

Lorella Pasquinucci
Carmela Parenti
M. Carmen Ruiz-Cantero
Zafiroula Georgoussi
Paschalina Pallaki
Enrique J. Cobos
Emanuele Amata
Agostino Marrazzo
Orazio Prezzavento
Emanuela Arena
Maria Dichiara
Loredana Salerno
Rita Turnaturi

Modifications at the basic nitrogen of the benzomorphan scaffold allowed the development of compounds able to segregate physiological responses downstream of the receptor signaling, opening new possibilities in opioid drug development. Alkylation of the phenyl ring in the N-substituent of the MOR-agonist/DOR-antagonist LP1 resulted in retention of MOR affinity. Moreover, derivatives 7a, 7c, and 7d were biased MOR agonists toward ERK1,2 activity stimulation, whereas derivative 7e was a low potency MOR agonist on adenylate cyclase inhibition. They were further screened in the mouse tail flick test and PGE2-induced hyperalgesia and drug-induced gastrointestinal transit.

Keywords:

Opioid
Pharmacology
Cyclase
Agonist
Hyperalgesia
Tail flick test
Benzomorphan
Stimulation
Antagonist
Biology

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