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首页> 外文期刊>Human Molecular Genetics >Sex-specific roles of beta-catenin in mouse gonadal development.
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Sex-specific roles of beta-catenin in mouse gonadal development.

机译:β-catenin在小鼠性腺发育中的性别特异性作用。

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Sexually dimorphic development of the gonads is controlled by positive and negative regulators produced by somatic cells. Many Wnt ligands, including ones that signal via the canonical beta-catenin pathway, are expressed in fetal gonads. beta-catenin, a key transcriptional regulator of the canonical Wnt pathway and an element of the cell adhesion complex, is essential for various aspects of embryogenesis. To study the involvement of beta-catenin in sex determination, we ablated beta-catenin specifically in the SF1-positive population of somatic cells. Although beta-catenin was present in gonads of both sexes, it was necessary only for ovarian differentiation but dispensable for testis development. Loss of beta-catenin in fetal testes did not affect Sertoli cell differentiation, testis morphogenesis or masculinization of the embryos. However, we observed molecular and morphological defects in ovaries lacking beta-catenin, including formation of testis-specific coelomic vessel, appearance of androgen-producing adrenal-like cells and loss of female germ cells. These phenotypes were strikingly similar to those found in the R-spondin1 (Rspo1) and Wnt4 knockout ovaries. In the absence of beta-catenin, expression of Wnt4 was down-regulated while that of Rspo1 was not affected, placing beta-catenin as a component in between Rspo1 and Wnt4. Our results demonstrate that beta-catenin is responsible for transducing sex-specific signals in the SF1-positive somatic cell population during mouse gonadal development.
机译:性腺的性二态性发育受体细胞产生的正负调节剂控制。许多Wnt配体(包括通过规范的β-catenin途径发出信号的配体)在胎儿性腺中表达。 β-catenin是经典Wnt途径的关键转录调节因子,是细胞粘附复合物的一个元素,对于胚胎发生的各个方面都是必不可少的。为了研究β-catenin在性别决定中的参与,我们专门消灭了体细胞SF1阳性人群中的β-catenin。尽管男女性腺中都存在β-catenin,但这仅对于卵巢分化是必需的,而对于睾丸发育却是必不可少的。胎儿睾丸中β-catenin的丢失不影响支持细胞分化,睾丸形态发生或胚胎的男性化。但是,我们观察到卵巢中缺乏β-catenin的分子和形态缺陷,包括睾丸特异的结肠血管的形成,产生雄激素的肾上腺样细胞的出现和雌性生殖细胞的丢失。这些表型与R-spondin1(Rspo1)和Wnt4敲除卵巢中的表型惊人地相似。在没有β-catenin的情况下,Wnt4的表达下调,而Rspo1的表达不受影响,将β-catenin作为Rspo1和Wnt4之间的组成部分。我们的结果表明,在小鼠性腺发育过程中,β-catenin负责转导SF1阳性体细胞群体中的性别特异性信号。

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