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Biochemical and functional characterization of high-affinity urotensin II receptors in rat cortical astrocytes
Authors:Castel Hélène  Diallo Mickaël  Chatenet David  Leprince Jérôme  Desrues Laurence  Schouft Marie-Thérèse  Fontaine Marc  Dubessy Christophe  Lihrmann Isabelle  Scalbert Elisabeth  Malagon Maria  Vaudry Hubert  Tonon Marie-Christine  Gandolfo Pierrick
Institution:INSERM, Laboratory of Cellular and Molecular Neuroendocrinology, European Institute for Peptide Research, University of Rouen, Mont-Saint-Aignan, France.
Abstract:The urotensin II (UII) gene is primarily expressed in the central nervous system, but the functions of UII in the brain remain elusive. Here, we show that cultured rat astrocytes constitutively express the UII receptor (UT). Saturation and competition experiments performed with iodinated rat UII ((125)I]rUII) revealed the presence of high- and low-affinity binding sites on astrocytes. Human UII (hUII) and the two highly active agonists hUII(4-11) and 3-iodo-Tyr9]hUII(4-11) were also very potent in displacing (125)I]rUII from its binding sites, whereas the non-cyclic analogue Ser5,10]hUII(4-11) and somatostatin-14 could only displace (125)I]rUII binding at micromolar concentrations. Reciprocally, rUII failed to compete with (125)I-Tyr0,D-Trp8]somatostatin-14 binding on astrocytes. Exposure of cultured astrocytes to rUII stimulated (3)H]inositol incorporation and increased intracellular Ca(2+) concentration in a dose-dependent manner. The stimulatory effect of rUII on polyphosphoinositide turnover was abolished by the phospholipase C inhibitor U73122, but only reduced by 56% by pertussis toxin. The GTP analogue Gpp(NH)p caused its own biphasic displacement of (125)I]rUII binding and provoked an affinity shift of the competition curve of rUII. Pertussis toxin shifted the competition curve towards a single lower affinity state. Taken together, these data demonstrate that rat astrocytes express high- and low-affinity UII binding sites coupled to G proteins, the high-affinity receptor exhibiting the same pharmacological and functional characteristics as UT.
Keywords:astrocytes  G-protein-coupled receptor  urotensin II  urotensin II receptor
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