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表达人生长激素基因的转基因小鼠为研究非肿瘤源性垂体细胞中人生长激素的合成和分泌提供了一个模型系统:地塞米松和甲状腺激素的不同作用。

Transgenic mice expressing the human growth hormone gene provide a model system to study human growth hormone synthesis and secretion in non-tumor-derived pituitary cells: differential effects of dexamethasone and thyroid hormone.

机构信息

Department of Physiology, University of Manitoba, Canada.

出版信息

Mol Cell Endocrinol. 2011 Oct 15;345(1-2):48-57. doi: 10.1016/j.mce.2011.07.010. Epub 2011 Jul 12.

Abstract

Growth hormone (GH) is regulated by pituitary and hypothalamic factors as well as peripheral endocrine factors including glucocorticoids and thyroid hormone. Studies on human GH are limited largely to the assessment of plasma levels in endocrine disorders. Thus, insight into the regulation of synthesis versus secretion has come mainly from studies done on non-human GH and/or pituitary tumor cells. However, primate and non-primate GH gene loci have differences in their structure and, by extension, regulation. We generated transgenic (171hGH/CS-TG) mice containing the intact hGH1 gene and locus control region, including sequences required for integration-independent and preferential pituitary expression. Here, we show hGH co-localizes with mouse (m) GH in somatotrophs in situ and in primary pituitary cells. Dexamethasone treatment increased hGH and mGH, as well as GH releasing hormone (GHRH) receptor RNA levels, and hGH release was stimulated by GHRH treatment. By contrast, triiodothyronine decreased or had no effect on hGH and mGH production, respectively, and the negative effect on hGH was also seen in the presence of dexamethasone. Thus, 171hGH/CS-TG mouse pituitary cultures represent a model system to investigate hormonal control of hGH synthesis and secretion.

摘要

生长激素(GH)受垂体和下丘脑因素以及外周内分泌因素的调节,包括糖皮质激素和甲状腺激素。对人类 GH 的研究主要限于内分泌紊乱时对血浆水平的评估。因此,对合成与分泌的调节的了解主要来自于对非人类 GH 和/或垂体肿瘤细胞的研究。然而,灵长类和非灵长类 GH 基因座在结构上存在差异,因此,在调节上也存在差异。我们生成了含有完整 hGH1 基因和基因座控制区的转基因(171hGH/CS-TG)小鼠,其中包括整合非依赖性和优先垂体表达所需的序列。在这里,我们发现在原位和原代垂体细胞中,hGH 与鼠(m)GH 共定位于生长激素细胞中。地塞米松处理增加了 hGH 和 mGH 以及生长激素释放激素(GHRH)受体 RNA 水平,GHRH 处理刺激了 hGH 的释放。相比之下,三碘甲状腺原氨酸分别降低或对 hGH 和 mGH 的产生没有影响,并且在存在地塞米松的情况下,对 hGH 的负作用也可见。因此,171hGH/CS-TG 小鼠垂体培养物代表了一个研究激素对 hGH 合成和分泌的控制的模型系统。

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