Bacteriophage Inspired Growth-Decoupled Recombinant Protein Production in Escherichia coli

大肠杆菌 噬菌体 重组DNA 抄写(语言学) 生物 合成生物学 蛋白质生物合成 细胞生物学 计算生物学 生物化学 基因 语言学 哲学
作者
Patrick Stargardt,Lukas Feuchtenhofer,Monika Cserjan‐Puschmann,Gerald Striedner,Juergen Mairhofer
出处
期刊:ACS Synthetic Biology [American Chemical Society]
卷期号:9 (6): 1336-1348 被引量:53
标识
DOI:10.1021/acssynbio.0c00028
摘要

Modulating resource allocation in bacteria to redirect metabolic building blocks to the formation of recombinant proteins rather than biomass formation remains a grand challenge in biotechnology. Here, we present a novel approach for improved recombinant protein production (RPP) using Escherichia coli (E. coli) by decoupling recombinant protein synthesis from cell growth. We show that cell division and host mRNA transcription can be successfully inhibited by coexpression of a bacteriophage-derived E. coli RNA polymerase (RNAP) inhibitor peptide and that genes overtranscribed by the orthogonal T7 RNAP can finally account to >55% of cell dry mass (CDM). This RNAP inhibitor peptide binds the E. coli RNAP and therefore prevents σ-factor 70 mediated formation of transcriptional qualified open promoter complexes. Thereby, the transcription of σ-factor 70 driven host genes is inhibited, and metabolic resources can be exclusively utilized for synthesis of the protein of interest (POI). Here, we mimic the late phase of bacteriophage infection by coexpressing a phage-derived xenogeneic regulator that reprograms the host cell and thereby are able to significantly improve RPP under industrial relevant fed-batch process conditions at bioreactor scale. We have evaluated production of several different recombinant proteins at different scales (from microscale to 20 L fed-batch scale) and have been able to improve total and soluble proteins yields up to 3.4-fold in comparison to the reference expression system E. coli BL21(DE3). This novel approach for growth-decoupled RPP has profound implications for biotechnology and bioengineering and helps to establish more cost-effective and generic manufacturing processes for biologics and biomaterials.
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