Deakin University
Browse

File(s) under permanent embargo

Modification of the furan ring of salvinorin A: identification of a selective partial agonist at the kappa opioid receptor

Version 2 2024-06-12, 15:18
Version 1 2017-05-09, 15:05
journal contribution
posted on 2024-06-12, 15:18 authored by C Béguin, KK Duncan, TA Munro, DM Ho, W Xu, L-Y Liu-Chen, WA Carlezon, BM Cohen
In an effort to find novel agents which selectively target the kappa opioid receptor (KOPR), we modified the furan ring of the highly potent and selective KOPR agonist salvinorin A. Introduction of small substituents at C-16 was well tolerated. 12-epi-Salvinorin A, synthesized in four steps from salvinorin A, was a selective partial agonist at the KOPR. No clear SAR patterns were observed for C-13 aryl ketones. Introducing a hydroxymethylene group between C-12 and the furan ring was tolerated. Small C-13 esters and ethers gave weak KOPR agonists, while all C-13 amides were inactive. Finally, substitution of oxadiazoles for the furan ring abolished affinity for the KOPR. None of the compounds displayed any KOPR antagonism or any affinity for mu or delta opioid receptors.

History

Journal

Bioorganic and medicinal chemistry

Volume

17

Pagination

1370-1380

Location

England

ISSN

0968-0896

eISSN

1464-3391

Language

eng

Publication classification

CN.1 Other journal article

Issue

3

Publisher

Elsevier