Literature DB >> 19741018

Deletion of Frs2alpha from the ureteric epithelium causes renal hypoplasia.

Sunder Sims-Lucas1, Luise Cullen-McEwen, Veraragavan P Eswarakumar, David Hains, Kayle Kish, Brian Becknell, Jue Zhang, John F Bertram, Fen Wang, Carlton M Bates.   

Abstract

Fibroblast growth factor receptor 2 (Fgfr2) signaling is critical in maintaining ureteric branching architecture and mesenchymal stromal morphogenesis in the kidney. Fibroblast growth factor receptor substrate 2alpha (Frs2alpha) is a major docking protein for Fgfr2 with downstream targets including Ets variant (Etv) 4 and Etv5 in other systems. Furthermore, global deletion of Frs2alpha causes early embryonic lethality. The purpose of the study was to determine the role of Frs2alpha in mediating Fgfr2 signaling in the ureteric epithelium. To that end, we generated mice with conditional deletion of Frs2alpha in the ureteric epithelium (Frs2alpha(UB-/-)) and mice with point mutations in the Frs2alpha binding site of Fgfr2 (Fgfr2(LR/LR)). Frs2alpha(UB-/-) mice developed mild renal hypoplasia characterized by decreased ureteric branching morphogenesis but maintained normal overall branching architecture and had normal mesenchymal stromal development. Reduced nephron endowment in postnatal mutant mice was observed, corresponding with the reduction in branching morphogenesis. Furthermore, there were no apparent renal abnormalities in Fgfr2(LR/LR) mice. Interestingly, Etv4 and Etv5 expression was unaltered in Frs2alpha(UB-/-) mice, as was Sprouty1, an antagonist of Frs2alpha signaling. However, Ret and Wnt11 (molecules critical for ureteric branching morphogenesis) mRNA levels were lower in mutants vs. controls. Taken together, these findings suggest that Fgfr2 signals through adapter molecules other than Frs2alpha in the ureteric epithelium. Furthermore, Frs2alpha may transmit signals through other receptor kinases present in ureteric epithelium. Finally, the renal hypoplasia observed in Frs2alpha(UB-/-) mice is likely secondary to decreased Ret and Wnt11 expression.

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Year:  2009        PMID: 19741018      PMCID: PMC2781346          DOI: 10.1152/ajprenal.00262.2009

Source DB:  PubMed          Journal:  Am J Physiol Renal Physiol        ISSN: 1522-1466


  46 in total

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Review 1.  To bud or not to bud: the RET perspective in CAKUT.

Authors:  T Keefe Davis; Masato Hoshi; Sanjay Jain
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2.  Ureteric morphogenesis requires Fgfr1 and Fgfr2/Frs2α signaling in the metanephric mesenchyme.

Authors:  Sunder Sims-Lucas; Valeria Di Giovanni; Caitlin Schaefer; Brian Cusack; Veraragavan P Eswarakumar; Carlton M Bates
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3.  Fibroblast growth factor receptor-Frs2α signaling is critical for nephron progenitors.

Authors:  Valeria Di Giovanni; Kenneth A Walker; Daniel Bushnell; Caitlin Schaefer; Sunder Sims-Lucas; Pawan Puri; Carlton M Bates
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Review 4.  Role of fibroblast growth factor receptor signaling in kidney development.

Authors:  Carlton M Bates
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Review 5.  Fibroblast growth factor receptor signaling in kidney and lower urinary tract development.

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Review 6.  Role of fibroblast growth factor receptor signaling in kidney development.

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7.  Fgfr1 and the IIIc isoform of Fgfr2 play critical roles in the metanephric mesenchyme mediating early inductive events in kidney development.

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8.  Independent roles of Fgfr2 and Frs2alpha in ureteric epithelium.

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Journal:  Development       Date:  2011-02-24       Impact factor: 6.868

Review 9.  Renin-angiotensin system in ureteric bud branching morphogenesis: insights into the mechanisms.

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