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通过“生物反应器进化”提高分批补料培养过程中哺乳动物细胞的性能。

Improving performance of mammalian cells in fed-batch processes through "bioreactor evolution".

作者信息

Prentice Holly L, Ehrenfels Barbara N, Sisk William P

机构信息

Biogen Idec, Inc., 14 Cambridge Center, Cambridge, Massachusetts 02142, USA.

出版信息

Biotechnol Prog. 2007 Mar-Apr;23(2):458-64. doi: 10.1021/bp060296y. Epub 2007 Feb 21.

Abstract

The amount of recombinant product obtained from mammalian cells grown in a bioreactor is in part limited by achievable cell densities and the ability of cells to remain viable over extended periods of time. In an attempt to generate cell lines capable of better bioreactor performance, we subjected the DG44 Chinese Hamster Ovary (CHO) host cell line and a recombinant production cell line to an iterative process whereby cells capable of surviving the harsh conditions in the bioreactor were selected. This selective process was termed "bioreactor evolution". Following the selective process, the "evolved" host cells attained a 2-fold increase in peak cell density and a 72% increase in integral cell area. Transient transfection experiments demonstrate that the evolved cells have the same transfection efficiency and the same secretory potential as the initial cells. The "evolved" host was also found to contain a large subpopulation of cells that did not require insulin for growth. From this, a new population of growth-factor-independent cells was obtained. These improvements in host properties should prove beneficial in the expression of recombinant proteins in fed-batch processes. The selective process was also applied to a recombinant production cell line. The evolved cells from this selection exhibited a 38% increase in peak cell density, a 30% increase in integral cell area, and a 36% increase in product titer. These increases were obtained without any appreciable impact on product quality, demonstrating the usefulness of this simple approach to improve the performance of recombinant cell lines.

摘要

在生物反应器中培养的哺乳动物细胞所获得的重组产物量,部分受到可达到的细胞密度以及细胞在较长时间内保持存活能力的限制。为了培育出能够在生物反应器中表现更佳的细胞系,我们对DG44中国仓鼠卵巢(CHO)宿主细胞系和一个重组生产细胞系进行了一个迭代过程,在此过程中,能够在生物反应器的恶劣条件下存活的细胞被筛选出来。这个筛选过程被称为“生物反应器进化”。经过筛选过程后,“进化后的”宿主细胞的峰值细胞密度增加了2倍,整体细胞面积增加了72%。瞬时转染实验表明,进化后的细胞与初始细胞具有相同的转染效率和分泌潜力。还发现“进化后的”宿主含有大量不需要胰岛素就能生长的细胞亚群。由此,获得了一批新的不依赖生长因子的细胞。宿主特性的这些改善在补料分批培养过程中重组蛋白的表达方面应该会被证明是有益的。这个筛选过程也应用于一个重组生产细胞系。从这个筛选中进化出的细胞峰值细胞密度增加了38%,整体细胞面积增加了30%,产物滴度增加了36%。这些增加在对产物质量没有任何明显影响的情况下实现,证明了这种简单方法在提高重组细胞系性能方面的有用性。

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