Publication | Open Access
Role of β-Catenin in Post-Meiotic Male Germ Cell Differentiation
46
Citations
67
References
2011
Year
SpermatogenesisGeneticsReproductive BiologyFertilisationEmbryologyReproductive EndocrinologyFemale InfertilityMale InfertilityGerm Cell DevelopmentGametogenesisPublic HealthGerm Cell DifferentiationGerm Cell FateGerm Cell BiologyInfertilityCell DivisionMeiosisGameteApical Es SurfaceTestis DevelopmentCell BiologyDevelopmental BiologyGerm CellMedicine
Though roles of β-catenin signaling during testis development have been well established, relatively little is known about its role in postnatal testicular physiology. Even less is known about its role in post-meiotic germ cell development and differentiation. Here, we report that β-catenin is highly expressed in post-meiotic germ cells and plays an important role during spermiogenesis in mice. Spermatid-specific deletion of β-catenin resulted in significantly reduced sperm count, increased germ cell apoptosis and impaired fertility. In addition, ultrastructural studies show that the loss of β-catenin in post-meiotic germ cells led to acrosomal defects, anomalous release of immature spermatids and disruption of adherens junctions between Sertoli cells and elongating spermatids (apical ectoplasmic specialization; ES). These defects are likely due to altered expression of several genes reportedly involved in Sertoli cell-germ cell adhesion and germ cell differentiation, as revealed by gene expression analysis. Taken together, our results suggest that β-catenin is an important molecular link that integrates Sertoli cell-germ cell adhesion with the signaling events essential for post-meiotic germ cell development and maturation. Since β-catenin is also highly expressed in the Sertoli cells, we propose that binding of germ cell β-catenin complex to β-catenin complex on Sertoli cell at the apical ES surface triggers a signaling cascade that regulates post-meiotic germ cell differentiation.
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