Department of Comparative Biosciences, University of Wisconsin-Madison, Madison, WI 53706, USA.
Dev Biol. 2013 Apr 15;376(2):125-35. doi: 10.1016/j.ydbio.2013.01.034. Epub 2013 Feb 8.
Fetal prostate development is initiated by androgens and patterned by androgen dependent and independent signals. How these signals integrate to control epithelial cell differentiation and prostatic bud patterning is not fully understood. To test the role of beta-catenin (Ctnnb1) in this process, we used a genetic approach to conditionally delete or stabilize Ctnnb1 in urogenital sinus (UGS) epithelium from which the prostate derives. Two opposing mechanisms of action were revealed. By deleting Ctnnb1, we found it is required for separation of UGS from cloaca, emergence or maintenance of differentiated UGS basal epithelium and formation of prostatic buds. By genetically inducing a patchy subset of UGS epithelial cells to express excess CTNNB1, we found its excess abundance increases Bmp expression and leads to a global impairment of prostatic bud formation. Addition of NOGGIN partially restores prostatic budding in UGS explants with excess Ctnnb1. These results indicate a requirement for Ctnnb1 in UGS basal epithelial cell differentiation, prostatic bud initiation and bud spacing and suggest some of these actions are mediated in part through activation of BMP signaling.
胎儿前列腺的发育由雄激素启动,并受到雄激素依赖和非依赖信号的调控。这些信号如何整合以控制上皮细胞分化和前列腺芽的形态发生尚未完全清楚。为了测试β-连环蛋白(Ctnnb1)在这个过程中的作用,我们使用了一种遗传方法,条件性地删除或稳定尿生殖窦(UGS)上皮细胞中的 Ctnnb1,前列腺就是从这里起源的。揭示了两种相反的作用机制。通过删除 Ctnnb1,我们发现它对于 UGS 与泄殖腔的分离、分化的 UGS 基底上皮的出现或维持以及前列腺芽的形成是必需的。通过遗传诱导 UGS 上皮细胞的一部分表达过量的 CTNNB1,我们发现其过量表达增加了 Bmp 的表达,并导致前列腺芽形成的全面受损。加入 NOGGIN 部分恢复了 UGS 外植体中过量 Ctnnb1 的前列腺芽形成。这些结果表明 Ctnnb1 对于 UGS 基底上皮细胞分化、前列腺芽起始和芽间距是必需的,并表明其中一些作用部分是通过激活 BMP 信号传导介导的。
