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人类生长激素释放因子在转基因小鼠中的表达导致体细胞生长增加。

Expression of human growth hormone-releasing factor in transgenic mice results in increased somatic growth.

作者信息

Hammer R E, Brinster R L, Rosenfeld M G, Evans R M, Mayo K E

出版信息

Nature. 1985;315(6018):413-6. doi: 10.1038/315413a0.

Abstract

The neurohumoral regulation of growth hormone secretion is mediated in part by two hypothalamic peptides that reach the anterior pituitary via the hypothalamo-hypophysial portal blood system. Somatostatin inhibits the release of growth hormone, whereas growth hormone-releasing factor (GRF) positively regulates both growth hormone synthesis and secretion. Two forms of human GRF, 40 and 44 amino acids long, have been characterized from extra-hypothalamic tumours as well as from the hypothalamus. Analysis of human GRF complementary DNA and genomic clones indicates that the GRF peptides are first synthesized as a 107- or 108-amino-acid precursor protein. To examine the physiological consequences of GRF expression, we have established strains of transgenic mice containing a fusion gene including the promoter/regulatory region of the mouse metallothionein-I (MT-I) gene and the coding region of the human GRF gene. We report that expression of the human GRF precursor protein in these animals results in measurable levels of human GRF and increased levels of mouse growth hormone in plasma and accelerated growth rates relative to control littermates. These results demonstrate a direct role for GRF in the positive regulation of somatic growth. Unexpectedly, female transgenic mice carrying the MT-GRF fusion gene are fertile, in contrast to female transgenic mice expressing human or rat growth hormone, which are generally infertile. These transgenic mouse strains should provide useful animal models for the study of several types of human growth disorders.

摘要

生长激素分泌的神经体液调节部分是由两种下丘脑肽介导的,它们通过下丘脑 - 垂体门脉血液系统到达垂体前叶。生长抑素抑制生长激素的释放,而生长激素释放因子(GRF)则对生长激素的合成和分泌起正向调节作用。已从下丘脑外肿瘤以及下丘脑鉴定出两种形式的人GRF,分别由40和44个氨基酸组成。对人GRF互补DNA和基因组克隆的分析表明,GRF肽最初是以107或108个氨基酸的前体蛋白形式合成的。为了研究GRF表达的生理后果,我们建立了转基因小鼠品系,其包含一个融合基因,该融合基因包括小鼠金属硫蛋白-I(MT-I)基因的启动子/调节区域和人GRF基因的编码区域。我们报告说,这些动物中人GRF前体蛋白的表达导致血浆中人GRF水平可测,小鼠生长激素水平升高,并且相对于对照同窝小鼠生长速度加快。这些结果证明了GRF在体细胞生长的正向调节中起直接作用。出乎意料的是,携带MT-GRF融合基因的雌性转基因小鼠是可育的,这与表达人或大鼠生长激素的雌性转基因小鼠通常不育形成对比。这些转基因小鼠品系应该为研究几种类型的人类生长障碍提供有用的动物模型。

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