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Ping-pong amplification of a retroviral vector achieves high-level gene expression: human growth hormone production.

机译:逆转录病毒载体的乒乓扩增可实现高水平的基因表达:人类生长激素的产生。

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摘要

Retroviral vectors offer major advantages for gene transfer studies but have not been useful for producing proteins in large quantities. This deficiency has resulted in part from interference to superinfection, which limits the numbers of active proviruses in cells. Recently, we found that these vectors amplify when they are added as calcium phosphate precipitates to cocultures of cells that package retroviruses into ecotropic and amphotropic host range envelopes. Helper-free virions from either cell type can infect the other without interference, resulting in theoretically limitless back-and-forth (ping-pong) vector replication. In initial studies, however, amplifications of a vector that contained the human growth hormone gene ceased when the hormone produced was 0.3% or less of cellular protein synthesis. This limit was caused by two factors. First, recombinant shutoff viruses that are replication defective and encode envelope glycoproteins form at a low probability during any round of the vector replication cycle and these spread in cocultures, thereby establishing interference. Single cells in shutoff cocultures therefore synthesize both ecotropic and amphotropic envelope glycoproteins, and they release promiscuous (presumably hybrid) virions. The probability of forming shutoff viruses before the vector had amplified to a high multiplicity was reduced by using small cocultures. Second, cells with large numbers of proviruses are unhealthy and their proviral expression can be unstable. Stable expresser cell clones were obtained by selection. Thereby, cell lines were readily obtained that stably produce human growth hormone as 4 to 6% of the total protein synthesis. A ping-pong retroviral vector can be used for high-level protein production in vertebrate cells.
机译:逆转录病毒载体为基因转移研究提供了主要优势,但尚未用于大量生产蛋白质。这种缺陷部分是由于对超级感染的干扰所致,从而限制了细胞中活性原病毒的数量。最近,我们发现这些载体以磷酸钙沉淀的形式添加到将逆转录病毒包装成嗜性和两性宿主范围包膜的细胞共培养物中时会扩增。来自任何一种细胞类型的无辅助病毒体都可以感染另一种而不受干扰,从而在理论上实现了无限制的来回(乒乓)载体复制。然而,在最初的研究中,当产生的激素占细胞蛋白质合成的0.3%或更低时,包含人类生长激素基因的载体的扩增就停止了。此限制是由两个因素引起的。首先,在载体复制周期的任何一轮中,复制缺陷型且编码包膜糖蛋白的重组关闭病毒形成的可能性很小,并且它们在共培养物中传播,从而产生干扰。因此,关闭共培养中的单细胞合成亲嗜性和两性包膜糖蛋白,并且它们会释放混杂的(可能是杂种的)病毒体。通过使用小型共培养,可以降低载体扩增至高度多样性之前形成关闭病毒的可能性。第二,含有大量原病毒的细胞不健康,其原病毒表达可能不稳定。通过选择获得稳定的表达细胞克隆。由此,容易获得稳定地产生人生长激素的细胞系,其占总蛋白质合成的4%至6%。乒乓逆转录病毒载体可用于脊椎动物细胞中的高水平蛋白质生产。

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