Publication | Closed Access
Perturbation of RET signaling in the embryonic kidney
32
Citations
31
References
1999
Year
Ld GenesNephrologyRet-ig Fusion ProteinCellular PhysiologyEmbryologyEmbryonic KidneyTissue DevelopmentSignaling PathwayKidney Tubule RemodelingCell SignalingRet-ig TreatmentMolecular PhysiologyMorphogenesisEmbryonic DevelopmentRenal PathophysiologyCell BiologyDevelopmental BiologySignal TransductionMedicineCell DevelopmentKidney Research
We have used a RET-Ig fusion protein to disrupt signaling in the rat embryonic kidney development pathway. Treatment of embryonic kidney organ cultures with RET-Ig results in a decrease in branching of the ureteric bud and a down regulation in expression of the Wnt-11, Wnt-4, and ld genes. These data suggest that Wnt-11, Wnt-4, and ld function downstream of RET signaling in normal development. Expression of BMP-7, shh, and ptc were uneffected by RET-Ig treatment, implying that these genes are regulated independently of ret. We have also performed immunohistochemistry with a GFR alpha-1 specific polyclonal antisera to localize GFR alpha-1 protein expression in the developing kidney.
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