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Constitutive dimerization of human serotonin 5-HT4 receptors in living cells
Authors:Berthouze Magali  Ayoub Mohammed  Russo Olivier  Rivail Lucie  Sicsic Sames  Fischmeister Rodolphe  Berque-Bestel Isabelle  Jockers Ralf  Lezoualc'h Frank
Institution:Laboratoire de Cardiologie Cellulaire et Moléculaire, INSERM U-446, Chatenay-Malabry, France.
Abstract:Serotonin 5-HT4 receptor isoforms are G protein-coupled receptors (GPCRs) with distinct pharmacological properties and may represent a valuable target for the treatment of many human disorders. Here, we have explored the process of dimerization of human 5-HT4 receptor (h5-HT4R) by means of co-immunoprecipitation and bioluminescence resonance energy transfer (BRET). Constitutive h5-HT4(d)R dimer was observed in living cells and membrane preparation of CHO and HEK293 cells. 5-HT4R ligands did not influence the constitutive energy transfer of the h5-HT4(d)R splice variant in intact cells and isolated plasma membranes. In addition, we found that h5-HT4(d)R and h5-HT4(g)R which structurally differ in the length of their C-terminal tails were able to form constitutive heterodimers independently of their activation state. Finally, we found that coexpression of h5-HT4R and beta2-adrenergic receptor (beta2AR) led to their heterodimerization. Given the large number of h5-HT4R isoforms which are coexpressed in a same tissue, our results points out the complexity by which this 5-HTR sub-type mediates its biological effects.
Keywords:β2AR  β2-adrenergic receptor  BRET  bioluminescence resonance energy transfer  CHO  Chinese hamster ovary cells  DMEM  Dulbecco’s modified Eagle’s medium  FCS  foetal calf serum  GPCRs  G protein-coupled receptors  IB  immunoblot  IP  immunoprecipitation  5-HT  5-hydroxytryptamine  HEK293  human embryonic kidney 293 cells  h5-HT4R  human 5-HT4 receptor  MT1R  MT1 melatonin receptor  PAGE  polyacrylamide gel electropheris  RLuc  Renilla luciferase  SDS  sodium dodecyl sulfate  TM  transmembrane  YFP  yellow fluorescent protein
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