Literature DB >> 18612081

Germ line activation of the Tie2 and SMMHC promoters causes noncell-specific deletion of floxed alleles.

Willem J de Lange1, Carmen M Halabi, Andreas M Beyer, Curt D Sigmund.   

Abstract

Tissue-specific knockouts generated through Cre-loxP recombination have become an important tool to manipulate the mouse genome. Normally, two successive rounds of breeding are performed to generate mice carrying two floxed target-gene alleles and a transgene expressing Cre-recombinase tissue-specifically. We show herein that two promoters commonly used to generate endothelium-specific (Tie2) and smooth muscle-specific [smooth muscle myosin heavy chain (Smmhc)] knockout mice exhibit activity in the female and male germ lines, respectively. This can result in the inheritance of a null allele in the second generation that is not tissue specific. Careful experimental design is required therefore to ensure that tissue-specific knockouts are indeed tissue specific and that appropriate controls are used to compare strains.

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Year:  2008        PMID: 18612081      PMCID: PMC2574738          DOI: 10.1152/physiolgenomics.90284.2008

Source DB:  PubMed          Journal:  Physiol Genomics        ISSN: 1094-8341            Impact factor:   3.107


  17 in total

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2.  Smooth muscle-specific expression of the smooth muscle myosin heavy chain gene in transgenic mice requires 5'-flanking and first intronic DNA sequence.

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4.  Development of a smooth muscle-targeted cre recombinase mouse reveals novel insights regarding smooth muscle myosin heavy chain promoter regulation.

Authors:  C P Regan; I Manabe; G K Owens
Journal:  Circ Res       Date:  2000-09-01       Impact factor: 17.367

5.  Smooth muscle expression of Cre recombinase and eGFP in transgenic mice.

Authors:  H-B Xin; K-Y Deng; M Rishniw; G Ji; M I Kotlikoff
Journal:  Physiol Genomics       Date:  2002-09-03       Impact factor: 3.107

6.  Temporal Cre-mediated recombination exclusively in endothelial cells using Tie2 regulatory elements.

Authors:  Anne Forde; Rainer Constien; Hermann-Josef Gröne; Günter Hämmerling; Bernd Arnold
Journal:  Genesis       Date:  2002-08       Impact factor: 2.487

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9.  Uniform vascular-endothelial-cell-specific gene expression in both embryonic and adult transgenic mice.

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Authors:  Kyoichiro Tsuchiya; Jun Tanaka; Yu Shuiqing; Carrie L Welch; Ronald A DePinho; Ira Tabas; Alan R Tall; Ira J Goldberg; Domenico Accili
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6.  Knockout of Na+/Ca2+ exchanger in smooth muscle attenuates vasoconstriction and L-type Ca2+ channel current and lowers blood pressure.

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8.  Deletion of Adam10 in endothelial cells leads to defects in organ-specific vascular structures.

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9.  p53 functions in endothelial cells to prevent radiation-induced myocardial injury in mice.

Authors:  Chang-Lung Lee; Everett J Moding; Kyle C Cuneo; Yifan Li; Julie M Sullivan; Lan Mao; Iman Washington; Laura B Jeffords; Rafaela C Rodrigues; Yan Ma; Shiva Das; Christopher D Kontos; Yongbaek Kim; Howard A Rockman; David G Kirsch
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10.  Conditional Tek promoter-driven deletion of arginyltransferase in the germ line causes defects in gametogenesis and early embryonic lethality in mice.

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