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An Androgen-Inducible Proximal Tubule-Specific Cre-Recombinase Transgenic Model

机译:雄激素诱导的近端小管特异性Cre重组酶转基因模型

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摘要

To facilitate the study of renal proximal tubules, we generated a transgenic mouse strain expressing an improved Cre-recombinase (iCre) under the control of the kidney androgen regulated protein (KAP) promoter. The transgene was expressed in the kidney of male mice but not in female mice. Treatment of female transgenic mice with androgen induced robust expression of the transgene in the kidney. We confirmed the presence of Cre-recombinase activity and the cell-specificity by breeding the KAP2-iCRE mice with ROSA26 reporter mice. X-gal staining of kidney sections from male double transgenic mice showed robust staining in the epithelial cells of renal proximal tubules. β-galactosidase staining in female mice became evident in proximal tubules after administration of androgen. This model of inducible Cre-recombinase in the renal proximal tubule should provide a novel useful tool for studying the physiological significance of genes expressed in the renal proximal tubule. This has advantages of other current models where cre-recombinase expression is constitutive, not inducible.
机译:为促进对肾近端小管的研究,我们在肾雄激素调节蛋白(KAP)启动子的控制下产生了表达改进的Cre重组酶(iCre)的转基因小鼠品系。转基因在雄性小鼠的肾脏中表达,而在雌性小鼠中则不表达。用雄激素治疗雌性转基因小鼠会在肾脏中强烈表达该转基因。我们通过用ROSA26报告基因小鼠繁殖KAP2-iCRE小鼠,证实了Cre重组酶活性和细胞特异性的存在。来自雄性双转基因小鼠的肾脏切片的X-gal染色显示肾近端小管的上皮细胞有牢固的染色。雄激素给药后,雌性小鼠的β-半乳糖苷酶染色在近端小管中变得明显。肾近端小管中这种可诱导的Cre重组酶模型应该为研究在肾近端小管中表达的基因的生理意义提供一个新颖的有用工具。这具有cre-重组酶表达是组成型而不是诱导型的其他当前模型的优点。

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