Abstract

The mu-opioid receptor (MOR) is essential for the rewarding and analgesic properties of opiate drugs, such as heroin and morphine. Furthermore, the importance of MOR systems for reward and reinforcement processes, more broadly, are evident from the fact that MOR knockout mice show reduced reward for many different drugs of abuse (nicotine, cocaine, alcohol and cannabinoids) and also for natural rewards such as social interactions and food. A key question that will be addressed in this Component is how MOR subpopulations that are expressed in distinct cell-types and circuits contribute to opioid reinforcement behaviors, specifically self-administration of the opioid receptor agonist, remifentanil. Components I and II have created and fully described genetically modified mice (BACs, knockins and knockouts) that either express MOR only in discrete brain regions (testing """"""""sufficiency"""""""" for addiction behaviors) or mice with deletions of MOR in specific brain areas (testing """"""""necessity"""""""" for addiction behaviors). We will initially determine if there are specific alterations in the acquisition and incubation of remifentanil self-administration as a result of restricted MOR expression. We will test if striatal expression of MOR predominantly confined to the striosome or patch compartment of the striatum is """"""""sufficient"""""""" for opioid addictive behaviors. Conversely, mice that lack MOR in the striatal neurons will be evaluated to test for the """"""""necessity"""""""" of striatal receptors for these same behaviors. We will then focus on the cellular and molecular adaptations within striatal specific cell-types as a consequence of opioid self-administration. Approaches will use optogenetics, electrophysiology and a very novel application of single cell transcriptome analysis developed by Dr. Yi Sun within the E/T-Core. Together this information will provide phenotypic profiles of discrete striatal cell-types (D1 and D2) within specific striatal compartments (ventral/dorsal, striosome/matrix) with the view of identifying novel adaptive mechanisms that could lead to therapeutic strategies for amelioration of drug abuse behaviors.

Public Health Relevance

Many addiction behaviors are mediated by opioid systems. The studies outlined in this CSORDA Component will determine which opioid neural circuits mediate different behaviors associated with opioid addiction. The research will identify cellular and molecular adaptations to self-administered opioid within individual cells associated with reward. The long-term goal will be toward discovering new therapeutic targets for substance abuse disorders.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Specialized Center (P50)
Project #
2P50DA005010-26
Application #
8355400
Study Section
Special Emphasis Panel (ZDA1-EXL-T (02))
Project Start
Project End
Budget Start
2012-07-15
Budget End
2013-06-30
Support Year
26
Fiscal Year
2012
Total Cost
$247,731
Indirect Cost
$86,867

  Institution

Name
University of California Los Angeles
Department
Type
DUNS #
092530369
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

Severino, Amie; Chen, Wenling; Hakimian, Joshua K et al. (2018) Mu-opioid receptors in nociceptive afferents produce a sustained suppression of hyperalgesia in chronic pain. Pain 159:1607-1620
Ben Hamida, Sami; Mendonça-Netto, Sueli; Arefin, Tanzil Mahmud et al. (2018) Increased Alcohol Seeking in Mice Lacking Gpr88 Involves Dysfunctional Mesocorticolimbic Networks. Biol Psychiatry 84:202-212
Lee, Kevin; Vuong, Helen E; Nusbaum, David J et al. (2018) The gut microbiota mediates reward and sensory responses associated with regimen-selective morphine dependence. Neuropsychopharmacology 43:2606-2614
Maroteaux, G; Arefin, T M; Harsan, L-A et al. (2018) Lack of anticipatory behavior in Gpr88 knockout mice showed by automatized home cage phenotyping. Genes Brain Behav 17:e12473
Ehrlich, Aliza T; Semache, Meriem; Bailly, Julie et al. (2018) Mapping GPR88-Venus illuminates a novel role for GPR88 in sensory processing. Brain Struct Funct 223:1275-1296
Lalanne, L; Ayranci, G; Filliol, D et al. (2017) Kappa opioid receptor antagonism and chronic antidepressant treatment have beneficial activities on social interactions and grooming deficits during heroin abstinence. Addict Biol 22:1010-1021
Dagnew, Robel; Lin, Yin-Ying; Agatep, Jerikko et al. (2017) CerebraLux: a low-cost, open-source, wireless probe for optogenetic stimulation. Neurophotonics 4:045001
Boulos, Laura-Joy; Darcq, Emmanuel; Kieffer, Brigitte Lina (2017) Translating the Habenula-From Rodents to Humans. Biol Psychiatry 81:296-305
Lu, Xiao-Hong; Yang, X William (2017) Genetically-directed Sparse Neuronal Labeling in BAC Transgenic Mice through Mononucleotide Repeat Frameshift. Sci Rep 7:43915
Arefin, Tanzil Mahmud; Mechling, Anna E; Meirsman, Aura Carole et al. (2017) Remodeling of Sensorimotor Brain Connectivity in Gpr88-Deficient Mice. Brain Connect 7:526-540

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