Abstract

There is burgeoning evidence that at least some of the pharmacological effects of opioids are mediated via opioid receptors that are organized as dimers or oligomers. Moreover, it is now established that in some cases different types opioid receptors can associate with one another to form heterodimers. The possibility that heterodimers may modulate signal transduction pathways that are not identical to those mediated by monomeric or homodimeric opioid receptors is an intriguing possibility that may have a bearing on tolerance and physical dependence. For these reasons, the broad, long-term objective of this project is to investigate the role of opioid receptor dimerization through a multidisciplinary, coordinated approach. In project 1, pharmacologic tools will be designed and synthesized to identify the presence of mu-delta opioid receptor dimers. The design approach involves the simultaneous occupation of neighboring mu and delta recognition sites in a heterodimer by a single bivalent ligand that contains mu agonist and delta antagonist pharmacophores. Optimization of binding and function will be accomplished by varying the length of the spacer that links the pharmacophores. In project 2, the interaction between mu and delta opioid receptors will be investigated in cultured cells. The activities of the mu receptors will be examined at different levels of expressed delta receptors. The ability of mu-selective opioid agonists to inhibit the production of intracellular CAMP or stimulation of the ERK1/2 activities will be determined when the expressed delta opioid receptors are being activated or inactivated. The ability of mu opioid agonists to elicit cellular adaptive responses such as desensitization or receptor internalization during mu opioid receptor activation or inactivation will be examined. Project 3 involves the molecular simulation of different dimer structures in a variety of dimer interfaces. Each will be built and evaluated according to theoretical scoring functions taken from protein homology and long time-scale molecular dynamics calculations. Bivalent ligands that have been found experimentally to bridge the opioid recognition sites in opioid receptor dimers will be employed as """"""""molecular rulers"""""""" to provide information on the distance between binding sites. Chronic testing of the target compounds will be carried out in mice to determine if there are in vivo correlates with the in vitro data obtained in projects 1 and 2.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Program Projects (P01)
Project #
5P01DA015091-04
Application #
6881610
Study Section
Human Development Research Subcommittee (NIDA)
Program Officer
Rapaka, Rao
Project Start
2002-05-01
Project End
2007-04-30
Budget Start
2005-05-01
Budget End
2006-04-30
Support Year
4
Fiscal Year
2005
Total Cost
$692,246
Indirect Cost

  Institution

Name
University of Minnesota Twin Cities
Department
Pharmacology
Type
Schools of Pharmacy
DUNS #
555917996
City
Minneapolis
State
MN
Country
United States
Zip Code
55455

  Publications

Lenard, Natalie R; Daniels, David J; Portoghese, Philip S et al. (2007) Absence of conditioned place preference or reinstatement with bivalent ligands containing mu-opioid receptor agonist and delta-opioid receptor antagonist pharmacophores. Eur J Pharmacol 566:75-82
Daniels, David J; Lenard, Natalie R; Etienne, Chris L et al. (2005) Opioid-induced tolerance and dependence in mice is modulated by the distance between pharmacophores in a bivalent ligand series. Proc Natl Acad Sci U S A 102:19208-13
Daniels, David J; Kulkarni, Amol; Xie, Zhihua et al. (2005) A bivalent ligand (KDAN-18) containing delta-antagonist and kappa-agonist pharmacophores bridges delta2 and kappa1 opioid receptor phenotypes. J Med Chem 48:1713-6
Lenard, Natalie R; Roerig, Sandra C (2005) Development of antinociceptive tolerance and physical dependence following morphine i.c.v. infusion in mice. Eur J Pharmacol 527:71-6
Xie, Zhihua; Bhushan, Rashmi G; Daniels, David J et al. (2005) Interaction of bivalent ligand KDN21 with heterodimeric delta-kappa opioid receptors in human embryonic kidney 293 cells. Mol Pharmacol 68:1079-86
Law, Ping-Yee; Erickson-Herbrandson, Laurie J; Zha, Qin Q et al. (2005) Heterodimerization of mu- and delta-opioid receptors occurs at the cell surface only and requires receptor-G protein interactions. J Biol Chem 280:11152-64
Bhushan, Rashmi G; Sharma, Shiv K; Xie, Zhihua et al. (2004) A bivalent ligand (KDN-21) reveals spinal delta and kappa opioid receptors are organized as heterodimers that give rise to delta(1) and kappa(2) phenotypes. Selective targeting of delta-kappa heterodimers. J Med Chem 47:2969-72
Law, P Y; Loh, H H; Wei, L-N (2004) Insights into the receptor transcription and signaling: implications in opioid tolerance and dependence. Neuropharmacology 47 Suppl 1:300-11