a previously functional tetracycline-regulated transactivator fails to target gene expression to the bone以前功能tetracycline-regulated反式激活因子未能目标基因表达的骨头.pdfVIP
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a previously functional tetracycline-regulated transactivator fails to target gene expression to the bone以前功能tetracycline-regulated反式激活因子未能目标基因表达的骨头
Schmidt and Eriksson BMC Research Notes 2011, 4:282
/1756-0500/4/282
SHORT REPORT Open Access
A previously functional tetracycline-regulated
transactivator fails to target gene expression to
the bone
*
Eva Schmidt and Maria Eriksson
Abstract
Background: The tetracycline-controlled transactivator system is a powerful tool to control gene expression in vitro
and to generate consistent and conditional transgenic in vivo model organisms. It has been widely used to study
gene function and to explore pathological mechanisms involved in human diseases. The system permits the
regulation of the expression of a target gene, both temporally and quantitatively, by the application of tetracycline
or its derivative, doxycycline. In addition, it offers the possibility to restrict gene expression in a spatial fashion by
utilizing tissue-specific promoters to drive the transactivator.
Findings: In this study, we report our problems using a reverse tetracycline-regulated transactivator (rtTA) in a
transgenic mouse model system for the bone-specific expression of the Hutchinson-Gilford progeria syndrome
mutation. Even though prior studies have been successful utilizing the same rtTA, expression analysis of the
transactivator revealed insufficient activity for regulating the transgene expression in our system. The absence of
transactivator could not be ascribed to differences in genetic background because mice in a mixed genetic
background and in congenic mouse lines showed similar results.
Conclusions: The purpose of this study is to report our negative experience with previously functional
transactivator mice, to raise caution in the use of tet-based transgenic mouse lines and to reinforce the need for
controls to ensure the stable functionality of generated tetracycline-controlled tr
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