首页> 美国卫生研究院文献>PLoS Genetics >Rosa26-GFP Direct Repeat (RaDR-GFP) Mice Reveal Tissue- and Age-Dependence of Homologous Recombination in Mammals In Vivo
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Rosa26-GFP Direct Repeat (RaDR-GFP) Mice Reveal Tissue- and Age-Dependence of Homologous Recombination in Mammals In Vivo

机译:Rosa26-GFP直接重复(RaDR-GFP)小鼠揭示了体内哺乳动物体内重组的组织和年龄依赖性。

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摘要

Homologous recombination (HR) is critical for the repair of double strand breaks and broken replication forks. Although HR is mostly error free, inherent or environmental conditions that either suppress or induce HR cause genomic instability. Despite its importance in carcinogenesis, due to limitations in our ability to detect HR in vivo, little is known about HR in mammalian tissues. Here, we describe a mouse model in which a direct repeat HR substrate is targeted to the ubiquitously expressed Rosa26 locus. In the Rosa26 Direct Repeat-GFP (RaDR-GFP) mice, HR between two truncated EGFP expression cassettes can yield a fluorescent signal. In-house image analysis software provides a rapid method for quantifying recombination events within intact tissues, and the frequency of recombinant cells can be evaluated by flow cytometry. A comparison among 11 tissues shows that the frequency of recombinant cells varies by more than two orders of magnitude among tissues, wherein HR in the brain is the lowest. Additionally, de novo recombination events accumulate with age in the colon, showing that this mouse model can be used to study the impact of chronic exposures on genomic stability. Exposure to N-methyl-N-nitrosourea, an alkylating agent similar to the cancer chemotherapeutic temozolomide, shows that the colon, liver and pancreas are susceptible to DNA damage-induced HR. Finally, histological analysis of the underlying cell types reveals that pancreatic acinar cells and liver hepatocytes undergo HR and also that HR can be specifically detected in colonic somatic stem cells. Taken together, the RaDR-GFP mouse model provides new understanding of how tissue and age impact susceptibility to HR, and enables future studies of genetic, environmental and physiological factors that modulate HR in mammals.
机译:同源重组(HR)对于修复双链断裂和断裂的复制叉至关重要。尽管HR几乎没有错误,但抑制或诱导HR的固有条件或环境条件会导致基因组不稳定。尽管它在致癌作用中具有重要意义,但由于我们在体内检测HR的能力有限,因此对哺乳动物组织中HR知之甚少。在这里,我们描述了一种小鼠模型,其中直接重复的HR底物靶向到普遍表达的Rosa26基因座。在Rosa26直接重复GFP(RaDR-GFP)小鼠中,两个截短的EGFP表达盒之间的HR可以产生荧光信号。内部图像分析软件提供了一种定量完整组织内重组事件的快速方法,重组细胞的频率可以通过流式细胞仪进行评估。 11种组织之间的比较表明,重组细胞的频率在组织之间的变化幅度超过两个数量级,其中脑中的HR最低。此外,从头重组事件随着年龄的增长在结肠中累积,表明该小鼠模型可用于研究长期暴露对基因组稳定性的影响。暴露于N-甲基-N-亚硝基脲(一种类似于癌症化疗剂替莫唑胺的烷基化剂)表明,结肠,肝脏和胰腺对DNA损伤诱导的HR敏感。最后,对基础细胞类型的组织学分析表明,胰腺腺泡细胞和肝肝细胞会经历HR,而且在结肠体细胞中可以特异性检测到HR。两者合计,RaDR-GFP小鼠模型提供了对组织和年龄如何影响HR敏感性的新认识,并使将来对调节哺乳动物HR的遗传,环境和生理因素的研究成为可能。

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