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工业生产重组治疗药物在大肠杆菌中的应用及其最新进展。

Industrial production of recombinant therapeutics in Escherichia coli and its recent advancements.

机构信息

Cell Sciences & Technology, AMGEN Inc, Thousand Oaks, CA, USA.

出版信息

J Ind Microbiol Biotechnol. 2012 Mar;39(3):383-99. doi: 10.1007/s10295-011-1082-9. Epub 2012 Jan 18.

Abstract

Nearly 30% of currently approved recombinant therapeutic proteins are produced in Escherichia coli. Due to its well-characterized genetics, rapid growth and high-yield production, E. coli has been a preferred choice and a workhorse for expression of non-glycosylated proteins in the biotech industry. There is a wealth of knowledge and comprehensive tools for E. coli systems, such as expression vectors, production strains, protein folding and fermentation technologies, that are well tailored for industrial applications. Advancement of the systems continues to meet the current industry needs, which are best illustrated by the recent drug approval of E. coli produced antibody fragments and Fc-fusion proteins by the FDA. Even more, recent progress in expression of complex proteins such as full-length aglycosylated antibodies, novel strain engineering, bacterial N-glycosylation and cell-free systems further suggests that complex proteins and humanized glycoproteins may be produced in E. coli in large quantities. This review summarizes the current technology used for commercial production of recombinant therapeutics in E. coli and recent advances that can potentially expand the use of this system toward more sophisticated protein therapeutics.

摘要

近 30%的已批准的重组治疗蛋白是在大肠杆菌中生产的。由于其遗传特性明确、生长迅速且产量高,大肠杆菌已成为生物技术行业中表达非糖基化蛋白的首选和主力。大肠杆菌系统拥有丰富的知识和全面的工具,如表达载体、生产菌株、蛋白质折叠和发酵技术,这些都非常适合工业应用。该系统的不断发展满足了当前行业的需求,最近 FDA 批准的大肠杆菌生产的抗体片段和 Fc 融合蛋白就是最好的例证。更重要的是,最近在全长非糖基化抗体、新型菌株工程、细菌 N-糖基化和无细胞系统等复杂蛋白表达方面的进展进一步表明,复杂蛋白和人源化糖蛋白可能大量在大肠杆菌中生产。本文总结了目前在大肠杆菌中商业化生产重组治疗药物所使用的技术和最新进展,这些进展可能会扩大该系统在更复杂的蛋白治疗药物方面的应用。

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