Abstract

During the past funding period, we have established that opioid agonists could induce the cloned opioid receptors to couple to all the Gi/Go proteins with similar proteins with similar potencies. We have established also that there are receptors to couple to all the Gi/Go proteins with similar potencies. We have established also that there are distinct differences between mu- and delta-opioid receptor activation of similar second messengers such as adenylyl cyclase, and other cellular proteins could be involved in the signaling of these opioid receptors. Thus, it is our hypothesis that mu- and delta-opioid receptors utilize different G proteins for the regulation of the same effector and that this is due to the subtle differences within the receptor domains involved in G protein interaction and activation. It is also hypotheses that opioid receptor signaling is mediated via scaffolding of cellular proteins. By recruiting different cellular proteins such as RGS to the proximity of the receptor signaling complexes, the amplitude and duration of the signals can be modulated. Hence, in the current proposal, we will use the ecdysone mammalian-inducible expression system to alter the various G protein involved in the mu- and delta-opioid receptor signaling in the same clonal cell line. We will use the random saturation mutational analysis together with the Receptor Selection and Amplification Technology (RSAT) to pinpoint the domains involved in mu-and delta-opioid receptor-G protein interaction and activation. We will demonstrate the existing of opioid receptor signaling units, the signaling via protein scaffolding and will identify the cellular proteins involved in the scaffolding. We will the alter the contents of signaling units by the inducible expression system and examine the effects of such alteration on opioid receptor signaling. All these experiments are designed to address our overall objective of understanding the mechanism in which neuronal cells could integrate the signals transduced by the membrane receptors that utilize the same spectrum of second messenger systems. These proposed studies also could illuminate further the problem of tolerance and dependence since it is our hypothesis that tolerance and dependence development to the repeated use of the opioid drugs are the cellular compensatory responses to the signals being transduced. By modulating the amplitude and duration of the signals within the signaling units, it might be possible to alter the degree of tolerance and dependence.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Project (R01)
Project #
5R01DA007339-11
Application #
6378537
Study Section
Special Emphasis Panel (ZRG1-MDCN-5 (01))
Program Officer
Koustova, Elena
Project Start
1991-07-01
Project End
2004-06-30
Budget Start
2001-07-01
Budget End
2002-06-30
Support Year
11
Fiscal Year
2001
Total Cost
$235,090
Indirect Cost

  Institution

Name
University of Minnesota Twin Cities
Department
Pharmacology
Type
Schools of Medicine
DUNS #
168559177
City
Minneapolis
State
MN
Country
United States
Zip Code
55455

  Publications

Wang, Yan; Wang, Yan-Xia; Liu, Ting et al. (2015) ?-Opioid receptor attenuates A? oligomers-induced neurotoxicity through mTOR signaling. CNS Neurosci Ther 21:8-14
Wang, Yan; Ge, Yan-Hui; Wang, Yan-Xia et al. (2015) Modulation of mTOR Activity by ?-Opioid Receptor is Dependent upon the Association of Receptor and FK506-Binding Protein 12. CNS Neurosci Ther 21:591-8
Yan, Ying-Hui; Wang, Yan; Zhao, Lan-Xue et al. (2014) Role of FK506 binding protein 12 in morphine-induced ?-opioid receptor internalization and desensitization. Neurosci Lett 566:231-235
Qiu, Yu; Zhao, Wei; Wang, Yan et al. (2014) FK506-binding protein 12 modulates ?-opioid receptor phosphorylation and protein kinase C(?)-dependent signaling by its direct interaction with the receptor. Mol Pharmacol 85:37-49
Miller, Eric C; Zhang, Lei; Dummer, Benjamin W et al. (2012) Differential modulation of drug-induced structural and functional plasticity of dendritic spines. Mol Pharmacol 82:333-43
Zheng, Hui; Chu, Ji; Zhang, Yuhan et al. (2011) Modulating micro-opioid receptor phosphorylation switches agonist-dependent signaling as reflected in PKCepsilon activation and dendritic spine stability. J Biol Chem 286:12724-33
Qiu, Yu; Wang, Yan; Law, Ping-Yee et al. (2011) Cholesterol regulates micro-opioid receptor-induced beta-arrestin 2 translocation to membrane lipid rafts. Mol Pharmacol 80:210-8
Zheng, Hui; Zeng, Yan; Chu, Ji et al. (2010) Modulations of NeuroD activity contribute to the differential effects of morphine and fentanyl on dendritic spine stability. J Neurosci 30:8102-10
Zheng, Hui; Loh, Horace H; Law, Ping-Yee (2010) Agonist-selective signaling of G protein-coupled receptor: mechanisms and implications. IUBMB Life 62:112-9
Zheng, Hui; Chu, Ji; Zeng, Yan et al. (2010) Yin Yang 1 phosphorylation contributes to the differential effects of mu-opioid receptor agonists on microRNA-190 expression. J Biol Chem 285:21994-2002

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