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Impaired Islet Function in Commonly Used Transgenic Mouse Lines due to Human Growth Hormone Minigene Expression

机译:由于人类生长激素小基因表达,在常用的转基因小鼠品系中胰岛功能受损。

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摘要

The human growth hormone (hGH) minigene is frequently used in the derivation of transgenic mouse lines to enhance transgene expression. Although this minigene is present in the transgenes as a secondcistron, and thus not thought to be expressed, we found that three commonly used lines, Pdx1-Cre(Late), RIP-Cre, and MIP-GFP, each expressed significant amounts of hGH in pancreatic islets. Locally secreted hGH binds to prolactin receptors on β cells, activates STAT5 signaling, and induces pregnancy-like changes in gene expression, thereby augmenting pancreatic β cell mass and insulin content. In addition, islets of Pdx1-Cre(Late) mice have lower GLUT2 expression and reduced glucose-induced insulin release and are protected against the β cell toxin streptozotocin. These findings may be important when interpreting results obtained when these and other hGH minigene-containing transgenic mice are used.
机译:人类生长激素(hGH)小基因经常用于衍生转基因小鼠品系以增强转基因表达。尽管此小基因作为第二顺反子存在于转基因中,因此不被表达,但我们发现三种常用的系Pdx1-Cre(Late),RIP-Cre和MIP-GFP均表达大量的hGH。在胰岛。局部分泌的hGH与β细胞上的催乳激素受体结合,激活STAT5信号传导,并诱导类似基因的妊娠样变化,从而增加胰腺β细胞的质量和胰岛素含量。此外,Pdx1-Cre(Late)小鼠的胰岛具有较低的GLUT2表达并减少了葡萄糖诱导的胰岛素释放,并且受到了针对β细胞毒素链脲佐菌素的保护。当解释使用这些和其他含hGH小基因的转基因小鼠时获得的结果时,这些发现可能很重要。

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