Untangling dopamine-adenosine receptor assembly in experimental parkinsonism
Author(s) -
Víctor FernándezDueñas,
Jaume Taura,
Martin Cottet,
Maricel GómezSoler,
Marc LópezCano,
Catherine Ledent,
Masahiko Watanabe,
Eric Trinquet,
JeanPhilippe Pin,
Rafael Luján,
Thierry Durroux,
Francisco Ciruela
Publication year - 2014
Publication title -
disease models and mechanisms
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.327
H-Index - 83
eISSN - 1754-8411
pISSN - 1754-8403
DOI - 10.1242/dmm.018143
Subject(s) - dopamine receptor d2 , striatum , dopaminergic , dopamine , neuroscience , basal ganglia , adenosine a2a receptor , proximity ligation assay , dopamine receptor , immunoelectron microscopy , adenosine receptor , parkinsonism , receptor , biology , medicine , disease , central nervous system , immunohistochemistry , agonist
Parkinson's disease (PD) is a dopaminergic-related pathology in which functioning of the basal ganglia is altered. It has been postulated that a direct receptor-receptor interaction - i.e. of dopamine D2 receptor (D2R) with adenosine A2A receptor (A2AR) (forming D2R-A2AR oligomers) - finely regulates this brain area. Accordingly, elucidating whether the pathology prompts changes to these complexes could provide valuable information for the design of new PD therapies. Here, we first resolved a long-standing question concerning whether D2R-A2AR assembly occurs in native tissue: by means of different complementary experimental approaches (i.e. immunoelectron microscopy, proximity ligation assay and TR-FRET), we unambiguously identified native D2R-A2AR oligomers in rat striatum. Subsequently, we determined that, under pathological conditions (i.e. in a rat PD model), D2R-A2AR interaction was impaired. Collectively, these results provide definitive evidence for alteration of native D2R-A2AR oligomers in experimental parkinsonism, thus conferring the rationale for appropriate oligomer-based PD treatments.
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