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Improving human interferon-beta production in mammalian cell lines by insertion of an intronic sequence within its naturally uninterrupted gene

机译:通过将内含子序列插入天然不间断的基因中来改善哺乳动物细胞系中人干扰素的生产

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摘要

Human beta-interferon is used extensively as a therapeutic agent in a wide variety of diseases, ranging from multiple sclerosis to viral infections. At present, the most common source of interferon-beta is derived from CHO (Chinese-hamster ovary) cells. Interestingly, however, the IFNB gene is characterized by a lack of intronic sequences and therefore does not undergo splicing during its expression pathway. As nuclear processing of pre-mRNA molecules has often been demonstrated to improve production yields of recombinant molecules, we have inserted a heterologous intronic sequence at different positions within the IFNB gene and analysed its effects on protein production. The results obtained in the present study show that the position of intron insertion has profound effects on the expression levels of the IFNB gene and on the nuclear/cytoplasm distribution levels of its mRNA as determined by FISH (fluorescent in situ hybridization) analysis of stably transfected clones. In conclusion, our results provide additional evidence that insertion of intronic sequences may be used to improve protein expression efficiency also in molecules that do not normally undergo any splicing process.
机译:人β干扰素被广泛用作多种疾病的治疗剂,从多发性硬化症到病毒感染。目前,最常见的干扰素-β来源是CHO(中国仓鼠卵巢)细胞。然而,有趣的是,IFNB基因的特征在于缺乏内含子序列,因此在其表达途径中不进行剪接。由于通常已证明前mRNA分子的核加工可提高重组分子的生产效率,因此我们在IFNB基因内的不同位置插入了异源内含子序列,并分析了其对蛋白质生产的影响。通过稳定转染的FISH(荧光原位杂交)分析确定,内含子插入的位置对IFNB基因的表达水平及其mRNA的核/细胞质分布水平具有深远的影响。克隆。总之,我们的结果提供了其他证据,即内含子序列的插入也可用​​于改善通常不经过任何剪接过程的分子中的蛋白质表达效率。

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