Literature DB >> 19656174

Striatal GPR88 expression is confined to the whole projection neuron population and is regulated by dopaminergic and glutamatergic afferents.

Renaud Massart1, Jean-Philippe Guilloux, Virginie Mignon, Pierre Sokoloff, Jorge Diaz.   

Abstract

GPR88, an orphan G protein-coupled receptor, was designated Strg/GPR88 for striatum-specific G protein-coupled receptor (K. Mizushima et al. (2000)Genomics, 69, 314-321). In this study, we focused on striatal GPR88 protein localization using a polyclonal antibody. We established that the distribution of immunoreactivity in rat brain matched that of GPR88 transcripts and provided evidence for its exclusive neuronal expression. GPR88 protein is abundant throughout the striatum of rat and primate, with expression limited to the two subsets of striatal projection medium spiny neurons (MSNs) expressing preprotachykinin-substance P or preproenkephalin mRNAs. Ultrastructural immunolabelling revealed the GPR88 concentration at post-synaptic sites along the somatodendritic compartments of MSNs, with pronounced preference for dendrites and dendritic spines. The GPR88-rich expression, in both striatal output pathways, designates this receptor as a potential therapeutic target for diseases involving dysfunction of the basal ganglia, such as Parkinson's disease. Hence, we investigated changes of GPR88 expression in a model of Parkinson's disease (unilateral 6-hydroxydopamine-lesioned rats) following repeated L-DOPA treatment. In dopamine-depleted striatum, GPR88 expression was differentially regulated, i.e. decreased in striatopallidal and increased in striatonigral MSNs. L-DOPA treatment led to a normalization of GPR88 levels through dopamine D1 and D2 receptor-mediated mechanisms in striatopallidal and striatonigral MSNs, respectively. Moreover, the removal of corticostriatal inputs, by ibotenate infusion, downregulated GPR88 in striatopallidal MSNs. These findings provide the first evidence that GPR88 is confined to striatal MSNs and indicate that L-DOPA-mediated behavioural effects in hemiparkinsonian rats may involve normalization of striatal GPR88 levels probably through dopamine receptor-mediated mechanisms and modulations of corticostriatal pathway activity.

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Year:  2009        PMID: 19656174     DOI: 10.1111/j.1460-9568.2009.06842.x

Source DB:  PubMed          Journal:  Eur J Neurosci        ISSN: 0953-816X            Impact factor:   3.386


  36 in total

1.  Local inactivation of Gpr88 in the nucleus accumbens attenuates behavioral deficits elicited by the neonatal administration of phencyclidine in rats.

Authors:  M Ingallinesi; L Le Bouil; N Faucon Biguet; A Do Thi; C Mannoury la Cour; M J Millan; P Ravassard; J Mallet; R Meloni
Journal:  Mol Psychiatry       Date:  2014-08-26       Impact factor: 15.992

2.  GPR88 - a putative signaling molecule predominantly expressed in the striatum: Cellular localization and developmental regulation.

Authors:  Vincent Van Waes; Kuei Y Tseng; Heinz Steiner
Journal:  Basal Ganglia       Date:  2011-07-01

3.  GPR88 in A2A receptor-expressing neurons modulates locomotor response to dopamine agonists but not sensorimotor gating.

Authors:  A C Meirsman; A de Kerchove d'Exaerde; B L Kieffer; A-M Ouagazzal
Journal:  Eur J Neurosci       Date:  2017-08-02       Impact factor: 3.386

4.  Mice Lacking GPR88 Show Motor Deficit, Improved Spatial Learning, and Low Anxiety Reversed by Delta Opioid Antagonist.

Authors:  Aura C Meirsman; Julie Le Merrer; Lucie P Pellissier; Jorge Diaz; Daniel Clesse; Brigitte L Kieffer; Jérôme A J Becker
Journal:  Biol Psychiatry       Date:  2015-06-06       Impact factor: 13.382

5.  Effect of Substitution on the Aniline Moiety of the GPR88 Agonist 2-PCCA: Synthesis, Structure-Activity Relationships, and Molecular Modeling Studies.

Authors:  Chunyang Jin; Ann M Decker; Danni L Harris; Bruce E Blough
Journal:  ACS Chem Neurosci       Date:  2016-08-16       Impact factor: 4.418

6.  Synthesis, pharmacological characterization, and structure-activity relationship studies of small molecular agonists for the orphan GPR88 receptor.

Authors:  Chunyang Jin; Ann M Decker; Xi-Ping Huang; Brian P Gilmour; Bruce E Blough; Bryan L Roth; Yang Hu; Joseph B Gill; X Peter Zhang
Journal:  ACS Chem Neurosci       Date:  2014-05-14       Impact factor: 4.418

7.  Lack of anticipatory behavior in Gpr88 knockout mice showed by automatized home cage phenotyping.

Authors:  G Maroteaux; T M Arefin; L-A Harsan; E Darcq; S Ben Hamida; B L Kieffer
Journal:  Genes Brain Behav       Date:  2018-04-19       Impact factor: 3.449

8.  Balanced NMDA receptor activity in dopamine D1 receptor (D1R)- and D2R-expressing medium spiny neurons is required for amphetamine sensitization.

Authors:  Lisa R Beutler; Matthew J Wanat; Albert Quintana; Elisenda Sanz; Nigel S Bamford; Larry S Zweifel; Richard D Palmiter
Journal:  Proc Natl Acad Sci U S A       Date:  2011-02-22       Impact factor: 11.205

9.  Design, Synthesis, and Structure-Activity Relationship Studies of (4-Alkoxyphenyl)glycinamides and Bioisosteric 1,3,4-Oxadiazoles as GPR88 Agonists.

Authors:  Md Toufiqur Rahman; Ann M Decker; Tiffany L Langston; Kelly M Mathews; Lucas Laudermilk; Rangan Maitra; Weiya Ma; Emmanuel Darcq; Brigitte L Kieffer; Chunyang Jin
Journal:  J Med Chem       Date:  2020-11-18       Impact factor: 7.446

10.  Mapping GPR88-Venus illuminates a novel role for GPR88 in sensory processing.

Authors:  Aliza T Ehrlich; Meriem Semache; Julie Bailly; Stefan Wojcik; Tanzil M Arefin; Christine Colley; Christian Le Gouill; Florence Gross; Viktoriya Lukasheva; Mireille Hogue; Emmanuel Darcq; Laura-Adela Harsan; Michel Bouvier; Brigitte L Kieffer
Journal:  Brain Struct Funct       Date:  2017-11-06       Impact factor: 3.270
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