Laboratory of Developmental Genetics, Institute of Cytology and Genetics SB RAS, Novosibirsk, Russia, 630090.
Institute of Genetic Technologies, Novosibirsk State University, Novosibirsk, Russia, 630090.
Transgenic Res. 2022 Oct;31(4-5):525-535. doi: 10.1007/s11248-022-00319-5. Epub 2022 Aug 12.
In this work, we set out to create mice susceptible to the SARS-CoV-2 coronavirus. To ensure the ubiquitous expression of the human ACE2 gene we used the human EF1a promoter. Using pronuclear microinjection of the transgene construct, we obtained six founders with the insertion of the EF1a-hACE2 transgene, from which four independent mouse lines were established. Unfortunately, only one line had low levels of hACE2 expression in some organs. In addition, we did not detect the hACE2 protein in primary lung fibroblasts from any of the transgenic lines. Bisulfite sequencing analysis revealed that the EF1a promoter was hypermethylated in the genomes of transgenic animals. Extensive analysis of published works about transgenic animals indicated that EF1a transgenic constructs are frequently inactive. Thus, our case cautions against using the EF1a promoter to generate transgenic animals, as it is prone to epigenetic silencing.
在这项工作中,我们旨在创建易感染 SARS-CoV-2 冠状病毒的小鼠。为确保人类 ACE2 基因的普遍表达,我们使用了人类 EF1a 启动子。通过原核显微注射转基因构建体,我们获得了六个带有 EF1a-hACE2 转基因插入的创始者,从中建立了四条独立的小鼠品系。不幸的是,只有一条线在一些器官中具有低水平的 hACE2 表达。此外,我们没有在任何转基因系的原代肺成纤维细胞中检测到 hACE2 蛋白。亚硫酸氢盐测序分析表明,转基因动物基因组中的 EF1a 启动子发生了过度甲基化。对已发表的转基因动物作品的广泛分析表明,EF1a 转基因构建体经常失活。因此,我们的案例告诫不要使用 EF1a 启动子来生成转基因动物,因为它容易受到表观遗传沉默的影响。
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