Abstract

Chronic use of cocaine in humans results in long-lasting alterations in brain structure and function. In laboratory animals, repeated intermittent cocaine administration produces an augmented behavioral response to a subsequent challenge dose of the drug. This phenomenon, referred to as behavioral sensitization, may be important in cocaine craving, a central factor in many cases of drug relapse. The endogenous opioid peptide/receptor system has been implicated in cocaine sensitization. However, the role of the OFQ/N/ORL-1 receptor system has not been characterized in this phenomenon. Our preliminary data show that concomitant OFQ/N administration with cocaine blocks the development of cocaine sensitization and this action of OFQ/N is antagonized by J-113397, an ORL-1 receptor antagonist. Thus, the OFQ/N/ORL-1 receptor system plays an important role in blocking this phenomenon and may be a potential target to develop drugs with anti-craving activity. In order to characterize the neurobiological substrate for such an action of OFQ/N, we will elucidate the site of action of OFQ/N. Additionally, since OFQ/N or related drugs will be used to treat cocaine addicts, using sensitization as an animal model of drug craving, we will determine if OFQ/N could reverse an already existing sensitized response, a more clinically relevant issue. Our preliminary data also show that the level of hypothalamic OFQ/N increases after repeated cocaine treatment, indicating that the endogenous OFQ/N/ORL-1 receptor system may be altered during development of sensitization. Thus, using RIA and binding assays, we will measure levels of OFQ/N and its receptor after cocaine treatment in brain regions involved in cocaine craving. Using knockout mice, we will also study the development of sensitization in the absence of the ORL-1 receptor or OFQ/N. The studies proposed in this grant will elucidate the role of OFQ/N/ORL-1 receptor system in cocaine sensitization and possibly provide important and useful information toward developing possible treatments for cocaine addiction.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Project (R01)
Project #
5R01DA016682-02
Application #
6920048
Study Section
Neurobiology of Motivated Behavior Study Section (NMB)
Program Officer
Lin, Geraline
Project Start
2004-07-15
Project End
2007-06-30
Budget Start
2005-07-01
Budget End
2006-06-30
Support Year
2
Fiscal Year
2005
Total Cost
$172,500
Indirect Cost

  Institution

Name
Western University of Health Sciences
Department
Pharmacology
Type
Schools of Pharmacy
DUNS #
093373694
City
Pomona
State
CA
Country
United States
Zip Code
91766

  Publications

Lutfy, K; Parikh, D; Lee, D L et al. (2016) Prohormone convertase 2 (PC2) null mice have increased mu opioid receptor levels accompanied by altered morphine-induced antinociception, tolerance and dependence. Neuroscience 329:318-25
Tseng, Andy; Nguyen, Khanh; Hamid, Abdul et al. (2013) The role of endogenous beta-endorphin and enkephalins in ethanol reward. Neuropharmacology 73:290-300
Ren, Xiuhai; Lutfy, Kabirullah; Mangubat, Michael et al. (2013) Alterations in phosphorylated CREB expression in different brain regions following short- and long-term morphine exposure: relationship to food intake. J Obes 2013:764742
Nie, Ying; Ferrini, Monica G; Liu, Yanjun et al. (2013) Morphine treatment selectively regulates expression of rat pituitary POMC and the prohormone convertases PC1/3 and PC2. Peptides 47:99-109
Marquez, Paul; Hamid, Abdul; Lutfy, Kabirullah (2013) The role of NOP receptors in psychomotor stimulation and locomotor sensitization induced by cocaine and amphetamine in mice. Eur J Pharmacol 707:41-5
Mangubat, Michael; Lutfy, Kabirullah; Lee, Martin L et al. (2012) Effect of nicotine on body composition in mice. J Endocrinol 212:317-26
Nguyen, Alexander T; Marquez, Paul; Hamid, Abdul et al. (2012) The rewarding action of acute cocaine is reduced in ýý-endorphin deficient but not in ýý opioid receptor knockout mice. Eur J Pharmacol 686:50-4
Lutfy, Kabirullah; Aimiuwu, Otaren; Mangubat, Michael et al. (2012) Nicotine stimulates secretion of corticosterone via both CRH and AVP receptors. J Neurochem 120:1108-16
Parikh, Drupad; Hamid, Abdul; Friedman, Theodore C et al. (2011) Stress-induced analgesia and endogenous opioid peptides: the importance of stress duration. Eur J Pharmacol 650:563-7
Anghel, A; Jamieson, C A M; Ren, X et al. (2010) Gene expression profiling following short-term and long-term morphine exposure in mice uncovers genes involved in food intake. Neuroscience 167:554-66

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