4.7 Article

Wt1 negatively regulates β-catenin signaling during testis development

期刊

DEVELOPMENT
卷 135, 期 10, 页码 1875-1885

出版社

COMPANY BIOLOGISTS LTD
DOI: 10.1242/dev.018572

关键词

beta-catenin; Wt1; testis; sertoli cell; mouse

资金

  1. NCI NIH HHS [CA34936, CA16672, P01 CA034936, P30 CA016672] Funding Source: Medline
  2. NICHD NIH HHS [R37 HD030284, R01 HD030284, HD30284] Funding Source: Medline
  3. NIDDK NIH HHS [DK69599, R01 DK069599] Funding Source: Medline

向作者/读者索取更多资源

beta-Catenin, as an important effector of the canonical Wnt signaling pathway and as a regulator of cell adhesion, has been demonstrated to be involved in multiple developmental processes and tumorigenesis. beta-Catenin expression was found mainly on the Sertoli cell membrane starting from embryonic day 15.5 in the developing testes. However, its potential role in Sertoli cells during testis formation has not been examined. To determine the function of beta-catenin in Sertoli cells during testis formation, we either deleted beta-catenin or expressed a constitutively active form of beta-catenin in Sertoli cells. We found that deletion caused no detectable abnormalities. However, stabilization caused severe phenotypes, including testicular cord disruption, germ cell depletion and inhibition of Mullerian duct regression. beta-Catenin stabilization caused changes in Sertoli cell identity and misregulation of inter-Sertoli cell contacts. As Wt1 conditional knockout in Sertoli cells causes similar phenotypes to our stabilized beta-catenin mutants, we then investigated the relationship of Wt1 and beta-catenin in Sertoli cells and found Wt1 inhibits beta-catenin signaling in these cells during testis development. Wt1 deletion resulted in upregulation of beta-catenin expression in Sertoli cells both in vitro and in vivo. Our study indicates that Sertoli cell expression of beta-catenin is dispensable for testis development. However, the suppression of beta-catenin signaling in these cells is essential for proper testis formation and Wt1 is a negative regulator of beta-catenin signaling during this developmental process.

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