β-Fluorofentanyls are pH-Sensitive Mu Opioid Receptor Agonists

26 July 2019, Version 1
This content is a preprint and has not undergone peer review at the time of posting.

Abstract

The concept recently postulated by Stein and coworkers (Science 2017, 355, 966) that mu opioid receptor (MOR) agonists possessing amines with attenuated basicity show pH-dependent activity and can selectively act at damaged, low pH tissues has been additionally supported by in vitro studies reported here. We synthesized and tested analogs of fentanyl possessing one or two fluorine atoms at the beta position of the phenethylamine side chain, with additional fluorines optionally added to the benzene ring of the side chain. These compounds were synthesized in 1 to 3 steps from commercial building blocks. The novel bis-fluorinated analog RR-49 showed superior pH sensitivity, with full efficacy relative to DAMGO, but with 19-fold higher potency (EC50) in a MOR cAMP assay at pH 6.5 versus 7.4. Such compounds hold significant promise as analgesics for inflammatory pain with reduced abuse potential.

Keywords

Mu opioid receptor
mu opioid receptor agonist
pH sensitive
analgesics
fluorinated drugs

Supplementary materials

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2019 07 24 Fluorinated fentanyl SI
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