Abstract

The objective of the proposed research is to develop novel, selective, and potent ligands for the opiatereceptor-like receptor (ORL1). ORL1 has a primary structure closely related to the opiate receptors, mu, delta and kappa. Although it is clearly in the opiate receptor family, opioid ligands do not bind to this receptor, nor does receptor activation mediate analgesia in the same manner as the other family members. The physiological functions of ORL1 and its endogenous ligand, nociceptin/orphanin FQ (N/OFQ), are not well understood, but it is clear that receptor activation can modulate pain as well as other CNS-mediated responses. In addition, N/OFQ's ability to modulate dopamine release as well as morphine conditioned place preference suggests that a role for novel ORL1 ligands as both pain and addiction medications. This application describes a medicinal chemistry approach to the design and identification of small-molecule, high affinity, selective ORL1 agonists and antagonists, based on a novel potent lead compound designed in our laboratories using computer-assisted drug design and synthesis. Our approach provides a basis for structure activity relationship (SAR) and computer-assisted modeling studies designed to develop new ligands for ORL1 based on novel templates. The compounds to be synthesized will contain sufficient structural variability to sample the ORL1 receptor binding pocket and thus define a pharmacophore for ORL1 and to better understand the differences between opioid receptor and ORL1 binding. All compounds synthesized will be tested for binding affinity at ORL1 and opioid receptors on human receptors expressed in CHO cells. Functional activity will be determined in two in vitro assays: stimulation of [35S]GTPgammaS binding to CHO cell membranes, and inhibition of cAMP accumulation in intact cells. High affinity and selective compounds will be tested for N/OFQ-like or N/OFQ inhibitory activity in mice and rats in models of analgesia, modulation of opiate tolerance, and reinforcing effects of drugs of abuse, with the goal of developing these compounds into novel therapeutics as non-addicting, analgesics, anxiolytics, or drug abuse medications. These studies should provide an improved understanding of the structural requirements for ORL1-selective ligands and the similarities and differences between the ORL1 and opioid receptors. As a complement to our study of ORL function, we will also synthesize a known high affinity ORL ligand as a precursor for PET studies in collaboration with John Hopkins University.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Project (R01)
Project #
5R01DA014026-03
Application #
6655510
Study Section
Human Development Research Subcommittee (NIDA)
Program Officer
Rapaka, Rao
Project Start
2001-09-30
Project End
2005-08-31
Budget Start
2003-09-01
Budget End
2004-08-31
Support Year
3
Fiscal Year
2003
Total Cost
$505,658
Indirect Cost

  Institution

Name
Sri International
Department
Type
DUNS #
009232752
City
Menlo Park
State
CA
Country
United States
Zip Code
94025

  Publications

Kallupi, Marsida; Shen, Qianwei; de Guglielmo, Giordano et al. (2018) Buprenorphine requires concomitant activation of NOP and MOP receptors to reduce cocaine consumption. Addict Biol 23:585-595
Ferrari, Federica; Malfacini, Davide; Journigan, Blair V et al. (2017) In vitro pharmacological characterization of a novel unbiased NOP receptor-selective nonpeptide agonist AT-403. Pharmacol Res Perspect 5:
Ferrari, Federica; Cerlesi, Maria Camilla; Malfacini, Davide et al. (2016) In vitro functional characterization of novel nociceptin/orphanin FQ receptor agonists in recombinant and native preparations. Eur J Pharmacol 793:1-13
Asth, L; Ruzza, C; Malfacini, D et al. (2016) Beta-arrestin 2 rather than G protein efficacy determines the anxiolytic-versus antidepressant-like effects of nociceptin/orphanin FQ receptor ligands. Neuropharmacology 105:434-442
Toll, Lawrence; Bruchas, Michael R; Calo', Girolamo et al. (2016) Nociceptin/Orphanin FQ Receptor Structure, Signaling, Ligands, Functions, and Interactions with Opioid Systems. Pharmacol Rev 68:419-57
Zaveri, Nurulain T (2016) Nociceptin Opioid Receptor (NOP) as a Therapeutic Target: Progress in Translation from Preclinical Research to Clinical Utility. J Med Chem 59:7011-28
Arcuri, Ludovico; Viaro, Riccardo; Bido, Simone et al. (2016) Genetic and pharmacological evidence that endogenous nociceptin/orphanin FQ contributes to dopamine cell loss in Parkinson's disease. Neurobiol Dis 89:55-64
Lutfy, Kabirullah; Zaveri, Nurulain T (2016) The Nociceptin Receptor as an Emerging Molecular Target for Cocaine Addiction. Prog Mol Biol Transl Sci 137:149-81
Vang, Derek; Paul, Jinny A; Nguyen, Julia et al. (2015) Small-molecule nociceptin receptor agonist ameliorates mast cell activation and pain in sickle mice. Haematologica 100:1517-25
Zaveri, Nurulain T; Journigan, V Blair; Polgar, Willma E (2015) Discovery of the first small-molecule opioid pan antagonist with nanomolar affinity at mu, delta, kappa, and nociceptin opioid receptors. ACS Chem Neurosci 6:646-57

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