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转座子介导的转基因技术、转基因拯救以及啮齿类动物和兔的组织特异性基因表达。

Transposon-mediated transgenesis, transgenic rescue, and tissue-specific gene expression in rodents and rabbits.

机构信息

Institute of Laboratory Animal Science, University of Veterinary Medicine Vienna, Vienna, Austria.

出版信息

FASEB J. 2013 Mar;27(3):930-41. doi: 10.1096/fj.12-205526. Epub 2012 Nov 29.

Abstract

Germline transgenesis is an important procedure for functional investigation of biological pathways, as well as for animal biotechnology. We have established a simple, nonviral protocol in three important biomedical model organisms frequently used in physiological studies. The protocol is based on the hyperactive Sleeping Beauty transposon system, SB100X, which reproducibly promoted generation of transgenic founders at frequencies of 50-64, 14-72, and 15% in mice, rats, and rabbits, respectively. The SB100X-mediated transgene integrations are less prone to genetic mosaicism and gene silencing as compared to either the classical pronuclear injection or to lentivirus-mediated transgenesis. The method was successfully applied to a variety of transgenes and animal models, and can be used to generate founders with single-copy integrations. The transposon vector also allows the generation of transgenic lines with tissue-specific expression patterns specified by promoter elements of choice, exemplified by a rat reporter strain useful for tracking serotonergic neurons. As a proof of principle, we rescued an inborn genetic defect in the fawn-hooded hypertensive rat by SB100X transgenesis. A side-by-side comparison of the SB100X- and piggyBac-based protocols revealed that the two systems are complementary, offering new opportunities in genome manipulation.

摘要

生殖系转基因是功能研究生物途径以及动物生物技术的重要程序。我们在三个经常用于生理研究的重要生物医学模式生物中建立了一种简单的非病毒方案。该方案基于超活性 Sleeping Beauty 转座子系统 SB100X,该系统在小鼠、大鼠和兔子中分别以 50-64%、14-72%和 15%的频率重复地促进了转基因创始者的产生。与经典的原核注射或慢病毒介导的转基因相比,SB100X 介导的转基因整合不太容易发生遗传嵌合体和基因沉默。该方法已成功应用于多种转基因和动物模型,可用于生成具有单拷贝整合的创始者。转座子载体还允许通过选择的启动子元件生成具有组织特异性表达模式的转基因系,例如用于跟踪 5-羟色胺能神经元的大鼠报告株。作为原理验证,我们通过 SB100X 转基因拯救了 fawn-hooded 高血压大鼠的一种先天性遗传缺陷。SB100X 和 piggyBac 两种方案的并排比较表明,这两个系统是互补的,为基因组操作提供了新的机会。

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