Literature DB >> 15797971

Cardiac transgenesis with the tetracycline transactivator changes myocardial function and gene expression.

Diana T McCloskey1, Lynne Turnbull, Philip M Swigart, Alexander C Zambon, Sally Turcato, Shuji Joho, William Grossman, Bruce R Conklin, Paul C Simpson, Anthony J Baker.   

Abstract

The cardiac-specific tetracycline-regulated gene expression system (tet-system) is a powerful tool using double-transgenic mice. The cardiac alpha-myosin heavy chain promoter (alphaMHC) drives lifetime expression of a tetracycline-inhibited transcription activator (tTA). Crossing alphaMHC-tTA mice with mice containing a tTA-responsive promoter linked to a target gene yields double-transgenic mice having tetracycline-repressed expression of the target gene in the heart. Using the tet-system, some studies use nontransgenic mice for the control group, whereas others use single-transgenic alphaMHC-tTA mice. However, previous studies found that high-level expression of a modified activator protein caused cardiomyopathy. Therefore, we tested whether cardiac expression of tTA was associated with altered function of alphaMHC-tTA mice compared with wild-type (WT) littermates. We monitored in vivo and in vitro function and gene expression profiles for myocardium from WT and alphaMHC-tTA mice. Compared with WT littermates, alphaMHC-tTA mice had a greater heart-to-body weight ratio (approximately 10%), ventricular dilation, and decreased ejection fraction, suggesting mild cardiomyopathy. In vitro, submaximal contractions were greater compared with WT and were associated with greater myofilament Ca2+ sensitivity. Gene expression profiling revealed that the expression of 153 genes was significantly changed by >20% when comparing alphaMHC-tTA with WT myocardium. These findings demonstrate that introduction of the alphaMHC-tTA construct causes significant effects on myocardial gene expression and major functional abnormalities in vivo and in vitro. For studies using the tet-system, these results suggest caution in the use of controls, since alphaMHC-tTA myocardium differs appreciably from WT. Furthermore, the results raise the possibility that the phenotype conferred by a target gene may be influenced by the modified genetic background of alphaMHC-tTA myocardium.

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Year:  2005        PMID: 15797971     DOI: 10.1152/physiolgenomics.00016.2005

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


  20 in total

1.  Cardiac-specific NRAP overexpression causes right ventricular dysfunction in mice.

Authors:  Shajia Lu; Garland L Crawford; Justin Dore; Stasia A Anderson; Daryl Despres; Robert Horowits
Journal:  Exp Cell Res       Date:  2011-01-26       Impact factor: 3.905

2.  Pleiotropic phenotype of a genomic knock-in of an RGS-insensitive G184S Gnai2 allele.

Authors:  Xinyan Huang; Ying Fu; Raelene A Charbeneau; Thomas L Saunders; Douglas K Taylor; Kurt D Hankenson; Mark W Russell; Louis G D'Alecy; Richard R Neubig
Journal:  Mol Cell Biol       Date:  2006-09       Impact factor: 4.272

3.  Reversibility of adverse, calcineurin-dependent cardiac remodeling.

Authors:  Jeff M Berry; Vien Le; David Rotter; Pavan K Battiprolu; Bennett Grinsfelder; Paul Tannous; Jana S Burchfield; Michael Czubryt; Johannes Backs; Eric N Olson; Beverly A Rothermel; Joseph A Hill
Journal:  Circ Res       Date:  2011-06-23       Impact factor: 17.367

4.  Metabolic syndrome in mice induced by expressing a transcriptional activator in adipose tissue.

Authors:  Liwen Zhang; Yuchen Zhou; Amber Ying Zhu; Xiang-qing Li; Steven S Mundt; Ling Gao; JeanMarie Lisnock; Melba Hernandez; Magdalena Alonso-Galicia; Martin S Springer; Edward A O'Neill; Bruce L Daugherty; Oscar Puig
Journal:  Transgenic Res       Date:  2011-10-26       Impact factor: 2.788

5.  Functional significance of the discordance between transcriptional profile and left ventricular structure/function during reverse remodeling.

Authors:  Veli K Topkara; Kari T Chambers; Kai-Chien Yang; Huei-Ping Tzeng; Sarah Evans; Carla Weinheimer; Attila Kovacs; Jeffrey Robbins; Philip Barger; Douglas L Mann
Journal:  JCI Insight       Date:  2016-04-06

6.  A mouse model for spatial and temporal expression of HGF in the heart.

Authors:  Ilan Riess; Valentina Sala; Christian Leo; Marco Demaria; Stefano Gatti; Simona Gallo; Amandine Fitou; Ombretta Boero; Renzo Levi; Ivan Cuccovillo; Fabiola Molla; Noeleen De Angelis; Lidia Staszewsky; Roberto Latini; Tiziana Crepaldi
Journal:  Transgenic Res       Date:  2011-03-01       Impact factor: 2.788

7.  Differential Neurotoxicity Related to Tetracycline Transactivator and TDP-43 Expression in Conditional TDP-43 Mouse Model of Frontotemporal Lobar Degeneration.

Authors:  L Kukreja; R Shahidehpour; G Kim; J Keegan; K R Sadleir; T Russell; J Csernansky; M Mesulam; R J Vassar; L Wang; H Dong; C Geula
Journal:  J Neurosci       Date:  2018-05-28       Impact factor: 6.167

Review 8.  Lost in transgenesis: a user's guide for genetically manipulating the mouse in cardiac research.

Authors:  Jennifer Davis; Marjorie Maillet; Joseph M Miano; Jeffery D Molkentin
Journal:  Circ Res       Date:  2012-08-31       Impact factor: 17.367

9.  Intersectin 1 contributes to phenotypes in vivo: implications for Down's syndrome.

Authors:  Michael P Hunter; Marianela Nelson; Michael Kurzer; Xuerong Wang; Richard J Kryscio; Elizabeth Head; Graziano Pinna; John P O'Bryan
Journal:  Neuroreport       Date:  2011-10-26       Impact factor: 1.837

10.  Expression of a Gi-coupled receptor in the heart causes impaired Ca2+ handling, myofilament injury, and dilated cardiomyopathy.

Authors:  Diana T McCloskey; Sally Turcato; Guan-Ying Wang; Lynne Turnbull; Bo-Qing Zhu; Thomas Bambino; Anita P Nguyen; David H Lovett; Robert A Nissenson; Joel S Karliner; Anthony J Baker
Journal:  Am J Physiol Heart Circ Physiol       Date:  2007-10-26       Impact factor: 4.733
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