Non-canonical Wnt signaling regulates cell polarity in female reproductive tract development via van gogh-like 2

doi:10.1242/dev.034066

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First published online April 10, 2009
doi: 10.1242/10.1242/dev.034066

Development 136, 1559-1570 (2009)
Published by The Company of Biologists 2009

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Non-canonical Wnt signaling regulates cell polarity in female reproductive tract development via van gogh-like 2

Alysia L. vandenBerg and David A. Sassoon^*

Myology Group, UMR S 787 Inserm, Université Pierre et Marie Curie Paris VI, 105 bd de l'Hôpital, 75634 Paris Cedex 13, France.

^* Author for correspondence (e-mail: david.a.sassoon{at}gmail.com)

Accepted 3 March 2009

Wnt signaling effectors direct the development and adult remodelingof the female reproductive tract (FRT); however, the role ofnon-canonical Wnt signaling has not been explored in this tissue.The non-canonical Wnt signaling protein van gogh-like 2 is mutatedin loop-tail (Lp) mutant mice (Vangl2^Lp), which display defectsin multiple tissues. We find that Vangl2^Lp mutant uterine epitheliumdisplays altered cell polarity, concommitant with changes incytoskeletal actin and scribble (scribbled, Scrb1) localization.The postnatal mutant phenotype is an exacerbation of that seenat birth, exhibiting more smooth muscle and reduced stromalmesenchyme. These data suggest that early changes in cell polarityhave lasting consequences for FRT development. Furthermore,Vangl2 is required to restrict Scrb1 protein to the basolateralepithelial membrane in the neonatal uterus, and an accumulationof fibrillar-like structures observed by electron microscopyin Vangl2^Lp mutant epithelium suggests that mislocalization ofScrb1 in mutants alters the composition of the apical face ofthe epithelium. Heterozygous and homozygous Vangl2^Lp mutant postnataltissues exhibit similar phenotypes and polarity defects anddisplay a 50% reduction in Wnt7a levels, suggesting that the Vangl2^Lpmutation acts dominantly in the FRT. These studies demonstratethat the establishment and maintenance of cell polarity throughnon-canonical Wnt signaling are required for FRT development.

Key words: Vangl2, Wnt, Female reproductive tract, Uterus

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