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首页> 外文期刊>The Journal of Endocrinology: The Journal of the Society for Endocrinology >Origin of a rapidly evolving homeostatic control system programming testis function
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Origin of a rapidly evolving homeostatic control system programming testis function

机译:快速发展的稳态控制系统编程睾丸功能的起源

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Mammals share common strategies for regulating reproduction, including a conserved hypothalamic–pituitary–gonadal axis; yet, individual species exhibit differences in reproductive performance. In this report, we describe the discovery of a species-restricted homeostatic control system programming testis growth and function. Prl3c1 is a member of the prolactin gene family and its protein product (PLP-J) was discovered as a uterine cytokine contributing to the establishment of pregnancy. We utilized mouse mutagenesis of Prl3c1 and revealed its involvement in the regulation of the male reproductive axis. The Prl3c1 -null male reproductive phenotype was characterized by testiculomegaly and hyperandrogenism. The larger testes in the Prl3c1 -null mice were associated with an expansion of the Leydig cell compartment. Prl3c1 locus is a template for two transcripts ( Prl3c1 -v1 and Prl3c1-v2 ) expressed in a tissue-specific pattern. Prl3c1-v1 is expressed in uterine decidua, while Prl3c1-v2 is expressed in Leydig cells of the testis. 5′RACE, chromatin immunoprecipitation and DNA methylation analyses were used to define cell-specific promoter usage and alternative transcript expression. We examined the Prl3c1 locus in five murid rodents and showed that the testicular transcript and encoded protein are the result of a recent retrotransposition event at the Mus musculus Prl3c1 locus. Prl3c1-v1 encodes PLP-J V1 and Prl3c1-v2 encodes PLP-J V2. Each protein exhibits distinct intracellular targeting and actions. PLP-J V2 possesses Leydig cell-static actions consistent with the Prl3c1 -null testicular phenotype. Analysis of the biology of the Prl3c1 gene has provided insight into a previously unappreciated homeostatic setpoint control system programming testicular growth and function.
机译:哺乳动物共有共同的调节生殖的策略,包括保守的下丘脑-垂体-性腺轴。然而,个别物种在生殖性能上表现出差异。在这份报告中,我们描述了一个物种受限的稳态控制系统编程睾丸生长和功能的发现。 Prl3c1是催乳素基因家族的成员,其蛋白质产物(PLP-J)被发现是促成妊娠的子宫细胞因子。我们利用小鼠诱变的Prl3c1,并揭示了其参与男性生殖轴的调控。 Prl3c1-无效的男性生殖表型的特征是睾丸肥大和雄激素过多。 Prl3c1-null小鼠中较大的睾丸与Leydig细胞区室的扩张有关。 Prl3c1基因座是两个以组织特异性模式表达的转录本(Prl3c1-v1和Prl3c1-v2)的模板。 Prl3c1-v1在子宫蜕膜中表达,而Prl3c1-v2在睾丸的Leydig细胞中表达。使用5'RACE,染色质免疫沉淀和DNA甲基化分析来定义细胞特异性启动子的使用和替代转录表达。我们检查了五个啮齿动物中的Prl3c1基因座,并表明睾丸转录本和编码的蛋白质是最近在小家鼠Prl3c1基因座上发生逆转位事件的结果。 Prl3c1-v1编码PLP-J V1,Prl3c1-v2编码PLP-J V2。每种蛋白质均表现出独特的细胞内靶向作用。 PLP-J V2具有与Prl3c1-无效睾丸表型一致的Leydig细胞静态作用。 Prl3c1基因的生物学分析提供了对以前未认识到的稳态睾丸生长和功能编程稳态控制系统的见解。

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