Abstract

The opiate analgesic drug morphine (MOR) has been shown to relieve pain by mechanisms that include the release of neuronal histamine (HA) and the subsequent activation of HA receptors in the periaqueductal grey (PAG). HA is known to function as a neuromodulator substance in the central nervous system. The proposed studies will characterize the sites and mechanisms by which HA relieves pain, and search for novel, pain-relieving medications based on these mechanisms. The experiments will use the techniques of in vivo microdialysis, intracerebral injections, and nociceptive testing in rats. The following studies will be performed: 1) MOR increases the release of neuronal HA in the PAG. To determine the mechanisms of this response, the effects of selective opiate receptor agonists and antagonists will be studied on the release of HA in the PAG in vivo. 2) HA injections into the PAG induce pain-relieving (i.e. analgesic) responses and, at higher doses, pain-enhancing (i.e. hyperalgesic) responses. To discover the pharmacological mechanisms underlying the HA-induced changes in nociceptive threshold, the effects of selective HD agonists and HA antagonists will be studied after intracerebral administration into the PAG. The unique HA-like compound SKF92374 will also be studied, since this agent appears to induce analgesic, but not hyperalgesic responses by a previously undiscovered mechanism. 3) HA and MOR interact to produce synergistic analgesic responses. To characterize the nature of these interactions, quantitative antinociceptive studies will be performed with combinations of various doses of HA and MOR. In addition, the effects of antagonists selective for sub-types of opiate receptors and HA receptors will be studied on these responses in the presence of these MOR-HA combinations. In addition to these studies of the PAG, pilot studies suggest that HA may also be an antinociceptive mediator in the raphe magnus (RM, another brain stem structure known to be important in pain relief). To address this hypothesis, several of the experiments proposed above for the PAG will also be performed in the RM. These studies will clarify the mechanisms by which MOR relieves pain, enhance the understanding of histaminergic antinociceptive mechanisms, and may lead to the discovery of non-addicting, novel medications for the treatment of pain.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Project (R01)
Project #
5R01DA003816-13
Application #
2837846
Study Section
Human Development Research Subcommittee (NIDA)
Program Officer
Thomas, David D
Project Start
1984-07-01
Project End
2000-04-30
Budget Start
1999-01-01
Budget End
2000-04-30
Support Year
13
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Albany Medical College
Department
Pharmacology
Type
Schools of Medicine
DUNS #
City
Albany
State
NY
Country
United States
Zip Code
12208

  Publications

Reid, M Carrington; Ghesquiere, Angela; Kenien, Cara et al. (2017) Expanding palliative care's reach in the community via the elder service agency network. Ann Palliat Med 6:S104-S107
Reid, M Carrington; Henderson Jr, Charles R; Trachtenberg, Melissa A et al. (2017) Implementing a Pain Self-Management Protocol in Home Care: A Cluster-Randomized Pragmatic Trial. J Am Geriatr Soc 65:1667-1675
Kiosses, Dimitris N; Ravdin, Lisa D; Stern, Amy et al. (2017) Problem Adaptation Therapy for Pain (PATH-Pain): A Psychosocial Intervention for Older Adults with Chronic Pain and Negative Emotions in Primary Care. Geriatrics (Basel) 2:
Guerriero, Fabio; Bolier, Ruth; Van Cleave, Janet H et al. (2016) Pharmacological Approaches for the Management of Persistent Pain in Older Adults: What Nurses Need to Know. J Gerontol Nurs 42:49-57
Conroy, Jennie L; Nalwalk, Julia W; Phillips, James G et al. (2013) CC12, a P450/epoxygenase inhibitor, acts in the rat rostral, ventromedial medulla to attenuate morphine antinociception. Brain Res 1499:1-11
Hoerbelt, Paul; Nalwalk, Julia W; Phillips, James G et al. (2013) Antinociceptive activity of CC44, a biotinylated improgan congener. Eur J Pharmacol 714:464-71
VanAlstine, Melissa A; Hough, Lindsay B (2011) Effects of acetylenic epoxygenase inhibitors on recombinant cytochrome p450s. Drug Metab Dispos 39:1221-6
Hough, Lindsay B; Rice, Frank L (2011) H3 receptors and pain modulation: peripheral, spinal, and brain interactions. J Pharmacol Exp Ther 336:30-7
Albrecht, Phillip J; Nalwalk, Julia W; Hough, Lindsay B (2011) Efficacy of improgan, a non-opioid analgesic, in neuropathic pain. Brain Res 1424:32-7
Hough, Lindsay B; Nalwalk, Julia W; Yang, Jun et al. (2011) Brain P450 epoxygenase activity is required for the antinociceptive effects of improgan, a nonopioid analgesic. Pain 152:878-87

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