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The P2Y4 receptor forms homo-oligomeric complexes in several CNS and PNS neuronal cells
Authors:Nadia D’Ambrosi  Monia Iafrate  Fabrizio Vacca  Susanna Amadio  Alessandro Tozzi  Nicola B Mercuri  Cinzia Volonté
Institution:(1) Fondazione Santa Lucia, Rome, Italy;(2) Department of Neuroscience, University of Rome Tor Vergata, Rome, Italy;(3) C.N.R. Institute of Neurobiology and Molecular Medicine, Rome, Italy;(4) Fondazione Santa Lucia at CERC, Via del Fosso di Fiorano, 64-00143 Rome, Italy
Abstract:It is well established that several cell surface receptors interact with each other to form dimers and oligomers, which are essential for their activation. Since little is known about the quaternary structure of P2Y receptors, in the present work, we investigated the expression of the G-protein-coupled P2Y4 subunit as monomeric or higher-order complex protein. We examined both endogenously expressed P2Y4 subtype with the aid of specific anti-P2Y4 antiserum, and heterologously transfected P2Y4-tagged receptors with the use of antitag antibodies. In both cases, we found the P2Y4 receptor displaying molecular masses corresponding to monomeric, dimeric and oligomeric structures. Experiments performed in the absence of reducing agents demonstrated that there is a strict correlation among the multiple protein bands and that the multimeric forms are at least partially assembled by disulphide bonds. The direct demonstration of P2Y4 homodimerisation comes instead from co–transfection and differential co–immunoprecipitation experiments, with the use of differently tagged P2Y4 receptors and antitag antibodies. The structural propensity of the P2Y4 protein to form homo-oligomers may open the possibility of a novel regulatory mechanism of physiopathological functions for this and additional P2Y receptors.
Keywords:G-protein-coupled receptors  PC12 cells  purinergic receptor  receptor dimerisation  SH-SY5Y cells
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