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四环素系统在肾脏中用于诱导蛋白合成。

Use of the tetracycline system for inducible protein synthesis in the kidney.

作者信息

Gallagher Anna Rachel, Schönig Kai, Brown Nelson, Bujard Hermann, Witzgall Ralph

机构信息

Institute for Anatomy and Cell Biology I , University of Heidelberg, Germany.

出版信息

J Am Soc Nephrol. 2003 Aug;14(8):2042-51. doi: 10.1097/01.asn.0000079615.38843.4a.

DOI:10.1097/01.asn.0000079615.38843.4a
PMID:12874458
Abstract

The great advantage of the tetracycline-inducible system lies in its ability to address a large variety of biological questions in a time-dependent and tissue-specific manner. This study describes a transgenic mouse line, rTA(LAP)-1, which produces the reverse tetracycline transactivator under control of the liver activator protein (LAP) promoter. Two reporter lines with luciferase and LacZ reporter genes were used to demonstrate predominant expression in the kidney and liver when doxycycline was added to the drinking water. In the kidney, transgene expression was found primarily in cortical proximal tubules. No luciferase and beta-galactosidase activity was detected in mice without doxycycline in the drinking water, which attests to the tight control of this system. One of the advantages of the tet system lies in its reversibility, and indeed, a virtually complete remission of transgene activity in both the kidney and liver was observed when doxycycline was withdrawn. Also examined was transactivator activity during development by exposing the mothers producing the reverse transactivator to doxycycline before mating. Transgene activity was detected in newborn kidneys and liver, indicating that sufficient amounts of doxycycline had crossed the placental barrier. During nephron development, the LAP promoter appeared to be only active in the more mature proximal tubules. Finally, the rTA(LAP)-1 line was used to inducibly express the human PKD2 cDNA in proximal tubules of transgenic mice, but no cystic changes were detected, even after 6 mo of induction.

摘要

四环素诱导系统的巨大优势在于它能够以时间依赖性和组织特异性的方式解决各种各样的生物学问题。本研究描述了一种转基因小鼠品系rTA(LAP)-1,它在肝脏激活蛋白(LAP)启动子的控制下产生反向四环素反式激活因子。使用了两个带有荧光素酶和LacZ报告基因的报告品系来证明,当在饮用水中添加强力霉素时,在肾脏和肝脏中存在主要表达。在肾脏中,转基因表达主要在皮质近端小管中发现。在饮用水中没有强力霉素的小鼠中未检测到荧光素酶和β-半乳糖苷酶活性,这证明了该系统的严格控制。四环素系统的优势之一在于其可逆性,事实上,当停用强力霉素时,在肾脏和肝脏中都观察到转基因活性几乎完全缓解。还通过在交配前让产生反向反式激活因子的母鼠接触强力霉素来检查发育过程中的反式激活因子活性。在新生小鼠的肾脏和肝脏中检测到转基因活性,表明有足够量的强力霉素穿过了胎盘屏障。在肾单位发育过程中,LAP启动子似乎仅在更成熟的近端小管中活跃。最后,rTA(LAP)-1品系用于在转基因小鼠的近端小管中诱导表达人PKD2 cDNA,但即使在诱导6个月后也未检测到囊性变化。

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