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转录因子 NR4A2 在雌性垂体泌乳素细胞中驱动催乳素表达中发挥重要作用。

The Transcription Factor NR4A2 Plays an Essential Role in Driving Prolactin Expression in Female Pituitary Lactotropes.

机构信息

Department of Genetics, University of Pennsylvania, Philadelphia, PA.

Perelman School of Medicine, University of Pennsylvania, Philadelphia, PA.

出版信息

Endocrinology. 2020 May 1;161(5). doi: 10.1210/endocr/bqaa046.

Abstract

Differentiation of the hormone-producing cells of the pituitary represents an informative model of cell fate determination. The generation and maintenance of 2 pituitary lineages, the growth hormone (GH)- producing somatotropes and the prolactin (PRL)- producing lactotropes, are dependent on the pituitary-specific transcription factor, POU1F1. While POU1F1 is expressed in both cell types, and plays a role in activation of both the Gh and Prl genes, expression of Gh and Prl is restricted to somatotropes and lactotropes, respectively. These observations imply the existence of additional factors that contribute to the somatotrope and lactotrope identities and their hormone expressions. Prior transcriptome analysis of primary somatotropes and lactotropes isolated from the mouse pituitary identified enrichment of a transcription factor, Nr4a2, in the lactotropes. Nr4a2 was shown in a cell culture model to bind the Prl promoter at a position adjacent to Pou1f1 and to synergize with Pou1f1 in driving Prl transcription. Here we demonstrate in vivo the role of Nr4a2 as an enhancer of Prl expression by conditional gene inactivation of the Nr4a2 gene in mouse lactotropes. We demonstrate that nuclear orphan receptor transcription factor (NR4A2) binding at the Prl promoter is dependent on actions of POU1F1; while POU1F1 is essential to loading polymerase (Pol) II on the Prl promoter, Nr4a2 plays a role in enhancing Pol II release into the Prl gene body. These studies establish an in vivo role of Nr4a2 in enhancing Prl expression in mouse lactotropes, explore its mechanism of action, and establish a system for further study of the lactotrope lineage in the pituitary.

摘要

垂体激素产生细胞的分化代表了细胞命运决定的一个信息丰富的模型。两种垂体谱系(生长激素(GH)产生的生长激素细胞和催乳素(PRL)产生的催乳素细胞)的产生和维持依赖于垂体特异性转录因子 POUS1F1。虽然 POUS1F1 在这两种细胞类型中均有表达,并在激活 Gh 和 Prl 基因中发挥作用,但 Gh 和 Prl 的表达分别局限于生长激素细胞和催乳素细胞。这些观察结果表明,存在其他因素有助于生长激素细胞和催乳素细胞的身份及其激素表达。从鼠垂体分离的原代生长激素细胞和催乳素细胞的转录组分析之前已经鉴定出 Nr4a2 转录因子在催乳素细胞中丰富。在细胞培养模型中,Nr4a2 被显示在 Pou1f1 附近的 Prl 启动子上结合,并与 Pou1f1 协同驱动 Prl 转录。在这里,我们通过在鼠催乳素细胞中条件性基因失活 Nr4a2 基因,在体内证明了 Nr4a2 作为 Prl 表达增强子的作用。我们证明了核孤儿受体转录因子(NR4A2)在 Prl 启动子上的结合依赖于 POUS1F1 的作用;虽然 POUS1F1 对于将聚合酶(Pol)II 加载到 Prl 启动子上是必需的,但 Nr4a2 在增强 Pol II 进入 Prl 基因体的释放中发挥作用。这些研究确立了 Nr4a2 在增强鼠催乳素细胞中 Prl 表达的体内作用,探讨了其作用机制,并建立了进一步研究垂体催乳素谱系的系统。

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