Abstract

The objective of this project is to address the relationship between opioid binding sites and pharmacodynamic potency of opioid agonists. Opioid receptor density and opioid agonist potency can be reliably altered by opioid antagonists, opioid agonists and CNS stimulants (e.g., cocaine and amphetamine). It is important to examine the pharmacologic and biochemical consequences of these drug treatments since they include drugs of abuse and significant tools in the clinical management of pain and drug abuse. The proposed studies will explore the factors that mediate increases (upregulation) in opioid binding sites in the CNS. The effect of CNS stimulants and endocrine factors on opioid antagonist-induced upregulation will be studies. CNS stimulants and opioid agonists can also produce receptor upregulation. Studies will investigate the common mechanism that converge on opioid receptor upregulation. Parallel pharmacodynamic studies using receptor selective agonists, and standard opioid analgesics, will assess the functional consequences of receptor upregulation. Parallel pharmacodynamic studies using receptor selective agonists, and standard opioid analgesics, will assess the functional consequences of receptor changes. The relationship between receptors and pharmacodynamic response will also be examined in different species. These studies will build on the differences between the rat and mouse in terms of opioid potency and receptor characteristics. The differences in CNS stimulant potentiation of opioid agonist potency at mu and omega spinal cord and brain opioid receptors will be examined. We will assess in a simple in vitro system the mechanism by which CNS stimulants reliably increase opioid receptor density. The in vivo effects of CNS stimulants on opioid binding in the CNS will also be evaluated. We will examine alterations in opioid receptor-effector coupling using pertussis toxin, a bacterial toxin which interferes with opioid mediated effects. Using binding and pharmacodynamic assays, we will explore the effects of the toxin on opioid actions including analgesia, tolerance and toxicity mediated by specific opioid receptors. The overall goal is to probe the nature of opioid pharmacodynamics and receptor regulation. These studies will provide an opportunity to develop a more complete understanding of how opioid effects (analgesia, tolerance, dependence, toxicity), as well as the actions of cocaine and amphetamine, might be mediated. The proposed studies may increase understanding of the basic mechanisms of drug abuse and pain and may provide important practical information for developing new strategies for treatment.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Project (R01)
Project #
5R01DA004185-07
Application #
2117046
Study Section
Drug Abuse Biomedical Research Review Committee (DABR)
Project Start
1987-09-01
Project End
1994-08-31
Budget Start
1992-09-21
Budget End
1993-08-31
Support Year
7
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
St. John's University
Department
Other Health Professions
Type
Schools of Pharmacy
DUNS #
City
Queens
State
NY
Country
United States
Zip Code
11439

  Publications

Duttaroy, A; Shen, J; Shah, S et al. (1999) Opioid receptor upregulation in mu-opioid receptor deficient CXBK and outbred Swiss Webster mice. Life Sci 65:113-23
Duttaroy, A; Gregorio, G; Shah, S et al. (1998) Acute ethanol exposure decreases the analgesic potency of morphine in mice. Life Sci 62:PL35-41
Shen, J; Shah, S; Hsu, H et al. (1998) The effects of antisense to Gialpha2 on opioid agonist potency and Gialpha2 protein and mRNA abundance in the mouse. Brain Res Mol Brain Res 59:247-55
Shah, S; Breivogel, C; Selly, D et al. (1997) Time-dependent effects of in vivo pertussis toxin on morphine analgesia and G-proteins in mice. Pharmacol Biochem Behav 56:465-9
Shah, S; Duttaroy, A; Chen, B T et al. (1997) The effect of mu-opioid receptor antisense on morphine potency and antagonist-induced supersensitivity and receptor upregulation. Brain Res Bull 42:479-84
Sehba, F; Duttaroy, A; Shah, S et al. (1997) In vivo homologous regulation of mu-opioid receptor gene expression in the mouse. Eur J Pharmacol 339:33-41
Duttaroy, A; Kirtman, R; Farrell, F et al. (1997) The effect of cumulative dosing on the analgesic potency of morphine in mice. Pharmacol Biochem Behav 58:67-71
Shah, S; Duttaroy, A; Sehba, F et al. (1997) The effect of ethanol drinking on opioid analgesia and receptors in mice. Alcohol 14:361-6
Shen, J; Chan, K W; Chen, B T et al. (1997) The effect of in vivo ethanol consumption on cyclic AMP and delta-opioid receptors in mouse striatum. Brain Res 770:65-71
Yoburn, B C; Shah, S; Chan, K et al. (1995) Supersensitivity to opioid analgesics following chronic opioid antagonist treatment: relationship to receptor selectivity. Pharmacol Biochem Behav 51:535-9

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