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Split-CreERT2: Temporal Control of DNA Recombination Mediated by Split-Cre Protein Fragment Complementation

机译：Split-CreERT2：分裂Cre蛋白片段互补介导的DNA重组的时间控制。

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BackgroundDNA recombination technologies such as the Cre/LoxP system advance modern biological research by allowing conditional gene regulation in vivo. However, the precise targeting of a particular cell type at a given time point has remained challenging since spatial specificity has so far depended exclusively on the promoter driving Cre recombinase expression. We have recently established split-Cre that allows DNA recombination to be controlled by coincidental activity of two promoters, thereby increasing spatial specificity of Cre-mediated DNA recombination. To allow temporal control of split-Cre-mediated DNA recombination we have now extended split-Cre by fusing split-Cre proteins with the tamoxifen inducible ERT2 domain derived from CreERT2.

机译：背景技术DNA重组技术（例如Cre / LoxP系统）通过允许在体内进行条件基因调节来推进现代生物学研究。然而，由于空间特异性迄今为止仅取决于驱动Cre重组酶表达的启动子，因此在给定时间点精确靶向特定细胞类型仍然具有挑战性。我们最近建立了split-Cre，它允许通过两个启动子的同时活动来控制DNA重组，从而增加Cre介导的DNA重组的空间特异性。为了允许时间控制split-Cre介导的DNA重组，我们现在通过将split-Cre蛋白与源自CreERT2的他莫昔芬可诱导的ERT2结构域融合来扩展split-Cre。

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期刊名称 PLoS Clinical Trials
作者
Johannes Hirrlinger; Robert P. Requardt; Ulrike Winkler; Franziska Wilhelm; Christine Schulze; Petra G. Hirrlinger;
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年(卷),期 2009(4),12
年度 2009
页码 e8354
总页数 8
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专利

1. Temporal Control of Cre Recombinase-mediated in Vitro DNA Recombination by Tet-on Gene Expression System [J] . Zhong-Min GUO, Kang XU, Ying YUE, Acta Biochinica et Biophysica Sinica . 2005,第2期

机译：Tet-on基因表达系统对Cre重组酶介导的体外DNA重组的时间控制
2. Temporal Control of Cre Recombinase-mediated in Vitro DNA Recombination by Tet-on Gene Expression System [J] . Zhong-Min GUO, Kang XU, Ying YUE, 生物化学与生物物理学报：英文版 . 2005,第002期

机译：Tet-on基因表达系统对Cre重组酶介导的体外DNA重组的时间控制
3. Interaction of vaccinia virus complement control protein with human complement proteins: factor I-mediated degradation of C3b to iC3b1 inactivates the alternative complement pathway. [J] . Sahu A, Isaacs SN, Soulika AM, The Journal of Immunology: Official Journal of the American Association of Immunologists . 1998,第11期

机译：牛痘病毒补体控制蛋白与人补体蛋白的相互作用：因子I介导的C3b降解为iC3b1使其他补体途径失活。
4. Non-Invasive Studies of Proteins and DNA Fragments by SEC and SEC Coupling Methods [C] . Thorsten Hofe, Gunter Reinhold, Daniela Held PMSE Symposia . 2007

机译：SEC和SEC耦合方法对蛋白质和DNA片段的非侵入性研究
5. Control of Rad51 nucleoprotein filament formation in DNA double-strand break repair by homologous recombination. [D] . Fortin, Gary Scott. 2004

机译：通过同源重组控制DNA双链断裂修复中Rad51核蛋白细丝形成。
6. Genetic recombination and complementation between bacteriophage T7 and cloned fragments of T7 DNA. [O] . J L Campbell, C C Richardson, F W Studier 1978

机译：T7噬菌体与克隆的T7 DNA片段之间的遗传重组和互补。
7. Split-CreERT2: Temporal Control of DNA Recombination Mediated by Split-Cre Protein Fragment Complementation [O] . Hirrlinger, Johannes, Requardt, Robert P., Winkler, Ulrike, 2009

机译：Split-CreERT2：分裂Cre蛋白片段互补介导的DNA重组的时间控制。
8. FY05 LDRD Final Report Investigation of AAA+ Protein Machines that Participate in DNA Replication, Recombination, and in Response to DNA Damage LDRD Project Tracking Code: 04-LW-049 [R] . Sawicka, D., de Carvalho-Kavanagh, M. S., Barsky, D., 2006

机译：2005财年LDRD最终报告调查参与DNa复制，重组和DNa损伤的aaa +蛋白质机器LDRD项目跟踪代码：04-LW-049

Split-CreERT2: Temporal Control of DNA Recombination Mediated by Split-Cre Protein Fragment Complementation

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