Literature DB >> 10749566

Bone morphogenetic protein 4 regulates the budding site and elongation of the mouse ureter.

Y Miyazaki1, K Oshima, A Fogo, B L Hogan, I Ichikawa.   

Abstract

In the normal mouse embryo, Bmp4 is expressed in mesenchymal cells surrounding the Wolffian duct (WD) and ureter stalk, whereas bone morphogenetic protein (BMP) type I receptor genes are transcribed either ubiquitously (Alk3) or exclusively in the WD and ureter epithelium (Alk6). Bmp4 heterozygous null mutant mice display, with high penetrance, abnormalities that mimic human congenital anomalies of the kidney and urinary tract (CAKUT), including hypo/dysplastic kidneys, hydroureter, ectopic ureterovesical (UV) junction, and double collecting system. Analysis of mutant embryos suggests that the kidney hypo/dysplasia results from reduced branching of the ureter, whereas the ectopic UV junction and double collecting system are due to ectopic ureteral budding from the WD and accessory budding from the main ureter, respectively. In the cultured metanephros deprived of sulfated glycosaminoglycans (S-GAGs), BMP4-loaded beads partially rescue growth and elongation of the ureter. By contrast, when S-GAGs synthesis is not inhibited, BMP4 beads inhibit ureter branching and expression of Wnt 11, a target of glial cell-derived neurotrophic factor signaling. Thus, Bmp4 has 2 functions in the early morphogenesis of the kidney and urinary tract. One is to inhibit ectopic budding from the WD or the ureter stalk by antagonizing inductive signals from the metanephric mesenchyme to the illegitimate sites on the WD. The other is to promote the elongation of the branching ureter within the metanephros, thereby promoting kidney morphogenesis.

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Year:  2000        PMID: 10749566      PMCID: PMC377476          DOI: 10.1172/JCI8256

Source DB:  PubMed          Journal:  J Clin Invest        ISSN: 0021-9738            Impact factor:   14.808


  31 in total

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Journal:  Development       Date:  1995-05       Impact factor: 6.868

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  135 in total

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Authors:  Brigitte Lelongt; Pierre Ronco
Journal:  Pediatr Nephrol       Date:  2003-06-17       Impact factor: 3.714

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Authors:  Cathy Mendelsohn
Journal:  J Clin Invest       Date:  2004-04       Impact factor: 14.808

Review 3.  Development of the kidney medulla.

Authors:  Renfang Song; Ihor V Yosypiv
Journal:  Organogenesis       Date:  2012-01-01       Impact factor: 2.500

Review 4.  MicroRNAs: potential regulators of renal development genes that contribute to CAKUT.

Authors:  April K Marrone; Jacqueline Ho
Journal:  Pediatr Nephrol       Date:  2013-09-03       Impact factor: 3.714

5.  Ureteric morphogenesis requires Fgfr1 and Fgfr2/Frs2α signaling in the metanephric mesenchyme.

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Journal:  J Am Soc Nephrol       Date:  2012-01-26       Impact factor: 10.121

6.  Absence of canonical Smad signaling in ureteral and bladder mesenchyme causes ureteropelvic junction obstruction.

Authors:  Piyush Tripathi; Yinqiu Wang; Adam M Casey; Feng Chen
Journal:  J Am Soc Nephrol       Date:  2012-01-26       Impact factor: 10.121

7.  Ureteric branching morphogenesis in BMP4 heterozygous mutant mice.

Authors:  Jason E Cain; John F Bertram
Journal:  J Anat       Date:  2006-12       Impact factor: 2.610

8.  Eya 1 acts as a critical regulator for specifying the metanephric mesenchyme.

Authors:  Gangadharan Sajithlal; Dan Zou; Derek Silvius; Pin-Xian Xu
Journal:  Dev Biol       Date:  2005-08-15       Impact factor: 3.582

Review 9.  BMP signaling and its modifiers in kidney development.

Authors:  Ryuichi Nishinakamura; Masaji Sakaguchi
Journal:  Pediatr Nephrol       Date:  2013-11-12       Impact factor: 3.714

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Authors:  Ihor V Yosypiv
Journal:  Pediatr Nephrol       Date:  2008-10-29       Impact factor: 3.714

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