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Generation and characterization of dickkopf3 mutant mice
Authors:Barrantes Ivan del Barco  Montero-Pedrazuela Ana  Guadaño-Ferraz Ana  Obregon Maria-Jesus  Martinez de Mena Raquel  Gailus-Durner Valérie  Fuchs Helmut  Franz Tobias J  Kalaydjiev Svetoslav  Klempt Martina  Hölter Sabine  Rathkolb Birgit  Reinhard Claudia  Morreale de Escobar Gabriella  Bernal Juan  Busch Dirk H  Wurst Wolfgang  Wolf Eckhard  Schulz Holger  Shtrom Svetlana  Greiner Erich  Hrabé de Angelis Martin  Westphal Heiner  Niehrs Christof
Affiliation:Division of Molecular Embryology, Deutsches Krebsforschungszentrum, Im Neuenheimer Feld 280, D-69120 Heidelberg, Germany.
Abstract:dickkopf (dkk) genes encode a small family of secreted Wnt antagonists, except for dkk3, which is divergent and whose function is poorly understood. Here, we describe the generation and characterization of dkk3 mutant mice. dkk3-deficient mice are viable and fertile. Phenotypic analysis shows no major alterations in organ morphology, physiology, and most clinical chemistry parameters. Since Dkk3 was proposed to function as thyroid hormone binding protein, we have analyzed deiodinase activities, as well as thyroid hormone levels. Mutant mice are euthyroid, and the data do not support a relationship of dkk3 with thyroid hormone metabolism. Altered phenotypes in dkk3 mutant mice were observed in the frequency of NK cells, immunoglobulin M, hemoglobin, and hematocrit levels, as well as lung ventilation. Furthermore, dkk3-deficient mice display hyperactivity.
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