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体内对CRE重组酶的强力多西环素依赖性控制。

Stringent doxycycline dependent control of CRE recombinase in vivo.

作者信息

Schönig Kai, Schwenk Frieder, Rajewsky Klaus, Bujard Hermann

机构信息

Zentrum für Molekulare Biologie der Universität Heidelberg, Im Neuenheimer Feld 282, D-69120 Heidelberg, Germany.

出版信息

Nucleic Acids Res. 2002 Dec 1;30(23):e134. doi: 10.1093/nar/gnf134.

Abstract

The strategy of modulating gene activities in vivo via CRE/loxP recombination would greatly profit from subjecting the recombination event to an independent and stringent temporal control. Here, we describe a transgenic mouse line, LC-1, where the expression of the cre and luciferase gene is tightly controlled by the Tet system. Using the R26R mouse line as indicator for CRE activity, and mouse lines expressing tetracycline controlled transactivators (tTA/rtTA) in various tissues, we show that; (i) in the non-induced state CRE recombinase is tightly controlled throughout the development and adulthood of an animal; (ii) upon induction, efficient recombination occurs in the adult animal in all tissues where tTA/rtTA is present, including hepatocytes, kidney cells, neurons and T lymphocytes; and (iii) no position effect appears to be caused by the LC-1 locus. Moreover, using the novel rTA(LAP)-1 mouse line, we show that in hepatocytes, complete deletion of the loxP-flanked insert in R26R animals is achieved less than 48 h after induction. Thus, the LC-1 mouse appears suitable for exploiting two rapidly increasing collections of mouse lines of which one provides tTA/rtTA in specific cell types/tissues, and the other a variety of loxP-flanked genes.

摘要

通过CRE/loxP重组在体内调节基因活性的策略将极大地受益于使重组事件受到独立且严格的时间控制。在此,我们描述了一种转基因小鼠品系LC-1,其中cre和荧光素酶基因的表达由Tet系统严格控制。使用R26R小鼠品系作为CRE活性的指示物,以及在各种组织中表达四环素调控反式激活因子(tTA/rtTA)的小鼠品系,我们表明:(i)在未诱导状态下,CRE重组酶在动物的整个发育和成年期均受到严格控制;(ii)诱导后,在成年动物中,在所有存在tTA/rtTA的组织(包括肝细胞、肾细胞、神经元和T淋巴细胞)中均发生高效重组;并且(iii)LC-1基因座似乎未引起位置效应。此外,使用新型rTA(LAP)-1小鼠品系,我们表明在肝细胞中,R26R动物中loxP侧翼插入片段在诱导后不到48小时即被完全删除。因此,LC-1小鼠似乎适用于利用两种迅速增加的小鼠品系集合,其中一种在特定细胞类型/组织中提供tTA/rtTA,另一种提供各种loxP侧翼基因。

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