L A Frohman, R D Kineman, J Kamegai, S Park, L T Teixeira, K T Coschigano, J J Kopchic
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Both models also have impaired responses to a GHS, implying an interaction between the two signaling systems. The spontaneous dwarf rat (SDR), in which a mutation of the GH gene results in total absence of the hormone, shows characteristic changes in the hypothalamic regulatory hormones due to an absence of GH feedback and alterations in the expression of each of their pituitary receptors. Treatment of SDRs with GHRH and a GHS has allowed demonstration of a stimulatory effect of GHRH on GHRH-R, GHS-R, and SRIF type 2 receptor (SSTR-2) expression and an inhibitory effect on SSTR-5 expression. GH also modifies the expression of these receptors, though its effects are seen at later time periods and appear to be indirect. Overall, the results indicate a complex regulation of GH secretion in which somatotrope receptor, as well as ligand expression, exerts an important physiological role. Both the SDR and the GH-R knockout (ko) mouse have small pituitaries and decreased somatotropes, despite elevated GHRH secretion and intact GHRH-R signaling. Introduction of the hGHRH transgene into GH-R ko mice confirmed that the proliferative effects of GHRH require GH/insulin-like growth factor-I (IGF-I) action. 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引用次数: 0
摘要
促生长功能需要考虑生长激素(GH)分泌和细胞增殖。这些过程的调节在很大程度上是由三种下丘脑激素控制的:GH释放激素(GHRH)、生长抑素(SRIF)和一种尚未确定的GH分泌激素(GHS)。每一种都与G蛋白连接的膜受体结合,信号通过细胞膜受体发生。我们的实验室使用了一系列的遗传和转基因模型,其中包括生长激素调节系统的单个成分的扰动,以研究生长激素信号传导和增殖。GHRH信号传导受损存在于有GHRH受体(R)突变的lit小鼠和有受体后信号传导缺陷的dw大鼠中。这两种模型对GHS的反应也受损,这意味着两个信号系统之间存在相互作用。自发性侏儒大鼠(SDR)的生长激素基因突变导致激素完全缺失,由于缺乏生长激素反馈和垂体受体表达的改变,下丘脑调节激素表现出特征性变化。用GHRH和GHS治疗sdr已经证明了GHRH对GHRH- r、GHS- r和SRIF 2型受体(SSTR-2)表达的刺激作用和对SSTR-5表达的抑制作用。生长激素也会改变这些受体的表达,尽管它的作用在较晚的时期才被发现,而且似乎是间接的。总的来说,结果表明生长激素分泌的复杂调控,其中生长激素受体以及配体表达发挥了重要的生理作用。SDR和GH-R敲除(ko)小鼠均有较小的垂体和降低的生长因子,尽管GHRH分泌升高和GHRH- r信号完整。将hGHRH转基因引入GH- r小鼠证实GHRH的增殖作用需要GH/胰岛素样生长因子- i (IGF-I)的作用。这些结果为研究参与生长斜体增殖的因素提供了新的见解。
Secretagogues and the somatotrope: signaling and proliferation.
Somatotrope function requires consideration of both growth hormone (GH) secretion and cellular proliferation. The regulation of these processes is, to a large extent, controlled by three hypothalamic hormones: GH-releasing hormone (GHRH), somatostatin (SRIF), and an as-yet-unidentified GH secretagogue (GHS). Each binds to G protein-linked membrane receptors through which signaling occurs. Our laboratory has used a series of genetic and transgenic models with perturbations of individual components of the GH regulatory system to study both somatotrope signaling and proliferation. Impaired GHRH signaling is present in the lit mouse, which has a GHRH receptor (R) mutation, and the dw rat, which has a post-receptor signaling defect. Both models also have impaired responses to a GHS, implying an interaction between the two signaling systems. The spontaneous dwarf rat (SDR), in which a mutation of the GH gene results in total absence of the hormone, shows characteristic changes in the hypothalamic regulatory hormones due to an absence of GH feedback and alterations in the expression of each of their pituitary receptors. Treatment of SDRs with GHRH and a GHS has allowed demonstration of a stimulatory effect of GHRH on GHRH-R, GHS-R, and SRIF type 2 receptor (SSTR-2) expression and an inhibitory effect on SSTR-5 expression. GH also modifies the expression of these receptors, though its effects are seen at later time periods and appear to be indirect. Overall, the results indicate a complex regulation of GH secretion in which somatotrope receptor, as well as ligand expression, exerts an important physiological role. Both the SDR and the GH-R knockout (ko) mouse have small pituitaries and decreased somatotropes, despite elevated GHRH secretion and intact GHRH-R signaling. Introduction of the hGHRH transgene into GH-R ko mice confirmed that the proliferative effects of GHRH require GH/insulin-like growth factor-I (IGF-I) action. The results offer new insights into factors participating in somatotrope proliferation.
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