Abstract

We plan to study the effects of chronic morphine exposure on the opioid receptors in the hippocampal region of the rat central nervous system (CNS). Our hypothesis is that cellular tolerance to chronic morphine exposure is the result of a reduction in opioid receptor coupling to its signal transduction system rather than a reduction in receptor affinity or receptor number. This proposal describes a series of experiments designed to test that hypothesis. Using extracellular electrophysiological recording methods, the opioid receptor types mediating the response of hippocampal pyramidal cells to morphine-like (opioid) compounds will be defined. Quantitative dose-effect relationships will be determined for selected opioid agonists to measure their potency changes in the morphine-tolerant hippocampal preparation. Using electrophysiological measures, the molecular basis for the reduction in agonist potency will be determined by comparing the opioid receptor affinities and agonist efficacies of selected opioids in hippocampal slices prepared from morphine-tolerant and drug-naive rats. This will require the adaptation of partial receptor inactivation methods originally developed for use in opioid sensitive smooth muscle bioassays. Using in vitro ligand binding assays selective for mu and delta sites, we will also compare the opioid receptor affinities and binding site densities in morphine-tolerant and naive rat hippocampus. If tolerance is a consequence of a change in the post receptor binding events as we predict, a likely site of change would be the coupling between the receptor and the signal transduction system. The proposed link between opioid receptors and GTP-coupling protein (Ni) will be determined by measuring the sensitivity of opioid effect to pertussis toxin treatment of the rat hippocampal slice. We will determine whether morphine-tolerance increases the pertussis toxin sensitivity as might be predicted by the expected change in agonist efficacy. The primary goal of these studies is an understanding of the cellular and molecular mechanisms used by the brain to adapt to chronic opiate exposure. Opiate addiction is known to have behavioral, cellular, and molecular components. Information will be obtained in this study to describe the latter mechanisms. By defining the specific molecular events underlying tolerance development in a model CNS system, we expect ultimately to have a clearer concept of the relevant clinical processes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Project (R01)
Project #
5R01DA004123-03
Application #
3209286
Study Section
Special Emphasis Panel (SRCD (25))
Project Start
1988-03-01
Project End
1991-02-28
Budget Start
1990-03-01
Budget End
1991-02-28
Support Year
3
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

Name
University of Washington
Department
Type
Schools of Medicine
DUNS #
135646524
City
Seattle
State
WA
Country
United States
Zip Code
98195

  Publications

Pirraglia, Paul A; Hampton, John M; Rosen, Allison B et al. (2011) Psychological distress and trends in healthcare expenditures and outpatient healthcare. Am J Manag Care 17:319-28
Drake, Carrie T; Chavkin, Charles; Milner, Teresa A (2007) Opioid systems in the dentate gyrus. Prog Brain Res 163:245-63
Chavkin, Charles; Sud, Sumit; Jin, Wenzhen et al. (2004) Salvinorin A, an active component of the hallucinogenic sage salvia divinorum is a highly efficacious kappa-opioid receptor agonist: structural and functional considerations. J Pharmacol Exp Ther 308:1197-203
Jin, Wenzhen; Zhang, Jianhua; Lou, Danwen et al. (2002) C-fos-deficient mouse hippocampal CA3 pyramidal neurons exhibit both enhanced basal and kainic acid-induced excitability. Neurosci Lett 331:151-4
Rogalski, S L; Chavkin, C (2001) Eicosanoids inhibit the G-protein-gated inwardly rectifying potassium channel (Kir3) at the Na+/PIP2 gating site. J Biol Chem 276:14855-60
Terman, G W; Eastman, C L; Chavkin, C (2001) Mu opiates inhibit long-term potentiation induction in the spinal cord slice. J Neurophysiol 85:485-94
Varnado-Rhodes, Y; Gunther, J; Terman, G W et al. (2000) Mu opioid analgesia and analgesic tolerance in two mouse strains: C57BL/6 and 129/SvJ. Proc West Pharmacol Soc 43:15-7
Chavkin, C (2000) Dynorphins are endogenous opioid peptides released from granule cells to act neurohumorly and inhibit excitatory neurotransmission in the hippocampus. Prog Brain Res 125:363-7
Terman, G W; Drake, C T; Simmons, M L et al. (2000) Opioid modulation of recurrent excitation in the hippocampal dentate gyrus. J Neurosci 20:4379-88
Kovoor, A; Celver, J; Abdryashitov, R I et al. (1999) Targeted construction of phosphorylation-independent beta-arrestin mutants with constitutive activity in cells. J Biol Chem 274:6831-4

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