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Tamoxifen Injection induce transient myocardiac dysfunction in mice

Tamoxifen Injection induce transient myocardiac dysfunction in mice
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摘要 Tamoxifen inducible cre-loxp system has been employed as a very powerful tool for cardiology research in mice. It enables researchers to control their interested gene expression in tight control in terms of tissue specification and time specification. Here, we reported that in the absence of loxp transgenes,tamoxifen injection can lead to myocardiac dysfunction 3 days after drug administration but cardiac function start recover from 2 days later. Tamoxifen inducible cre-loxp system has been employed as a very powerful tool for cardiology research in mice. It enables researchers to control their interested gene expression in tight control in terms of tissue specification and time specification. Here, we reported that in the absence of loxp transgenes,tamoxifen injection can lead to myocardiac dysfunction 3 days after drug administration but cardiac function start recover from 2 days later.
作者 Yan Yan Wang Sheng Liu Bin Yu
机构地区 Tian Jin University of Traditional Chinese Medicine Tian Jin Meidical University
出处 《生物技术世界》 2014年第3期99-101,共3页 Biotech World
关键词 TAMOXIFEN CARDIOLOGY ECHO Tamoxifen Cardiology echo
分类号 R965 [医药卫生—药理学]
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参考文献8

  • 1Kristin B. Andersson,Lisbeth H. Winer,Halvor K. M?rk,Jeffery D. Molkentin,Frédéric Jaisser.Tamoxifen administration routes and dosage for inducible Cre-mediated gene disruption in mouse hearts[J].Transgenic Research.2010(4)
  • 2Michael Bordonaro,Phillip Bird.Modular Cre/lox System and Genetic Therapeutics for Colorectal Cancer[J].Journal of Biomedicine and Biotechnology.2009
  • 3Norimichi Koitabashi,Djahida Bedja,Ari L. Zaiman,Yigal M. Pinto,Manling Zhang,Kathleen L. Gabrielson,Eiki Takimoto,David A. KassZ.Avoidance of Transient Cardiomyopathy in Cardiomyocyte-Targeted Tamoxifen-Induced MerCreMer Gene Deletion Models[J].Circulation Research.2009(1)
  • 4Takimoto, Eiki,Koitabashi, Norimichi,Hsu, Steven,Ketner, Elizabeth A,Zhang, Manling,Nagayama, Takahiro,Bedja, Djahida,Gabrielson, Kathleen L,Blanton, Robert,Siderovski, David P,Mendelsohn, Michael E,Kass, David A.Regulator of G protein signaling 2 mediates cardiac compensation to pressure overload and antihypertrophic effects of PDE5 inhibition in mice[J].Journal of Clinical Investigation.2009(2)
  • 5Jeffery D. Molkentin,Jeffrey Robbins.With great power comes great responsibility: Using mouse genetics to study cardiac hypertrophy and failure[J].Journal of Molecular and Cellular Cardiology.2008(2)
  • 6Eiki Takimoto,Hunter C. Champion,Diego Belardi,Javid Moslehi,Marco Mongillo,Evanthia Mergia,David C. Montrose,Takayoshi Isoda,Kate Aufiero,Manuela Zaccolo,Wolfgang R. Dostmann,Carolyn J. Smith,David A. Kass.cGMP Catabolism by Phosphodiesterase 5A Regulates Cardiac Adrenergic Stimulation by NOS3-Dependent Mechanism[J].Circulation Research.2005(1)
  • 7Dawinder S. Sohal,Mai Nghiem,Michael A. Crackower,Sandra A. Witt,Thomas R. Kimball,Kevin M. Tymitz,Josef M. Penninger,Jeffery D. Molkentin.Temporally Regulated and Tissue-Specific Gene Manipulations in the Adult and Embryonic Heart Using a Tamoxifen-Inducible Cre Protein[J].Circulation Research: Journal of the American Heart Association.2001(1)
  • 8Chrysi Verrou,Yong Zhang,Christa Zürn,Wolfgang W.A. Schamel,Michael Reth.Comparison of the Tamoxifen Regulated Chimeric CreRecombinases MerCreMer and CreMer[J].Biological Chemistry.1999(12)
生物技术世界
2014年 第3期

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