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重组生产的派罗西汀肽的经济高效下游加工及其抗菌活性。

Cost-effective downstream processing of recombinantly produced pexiganan peptide and its antimicrobial activity.

作者信息

Sun Baode, Wibowo David, Middelberg Anton P J, Zhao Chun-Xia

机构信息

Australian Institute for Bioengineering and Nanotechnology, The University of Queensland, St Lucia, QLD, 4072, Australia.

Faculty of Engineering, Computer, and Mathematical Sciences, The University of Adelaide, Adelaide, SA, 5005, Australia.

出版信息

AMB Express. 2018 Jan 24;8(1):6. doi: 10.1186/s13568-018-0541-3.

Abstract

Antimicrobial peptides (AMPs) have significant potential as alternatives to classical antibiotics. However, AMPs are currently prepared using processes which are often laborious, expensive and of low-yield, thus hindering their research and application. Large-scale methods for production of AMPs using a cost-effective approach is urgently required. In this study, we report a scalable, chromatography-free downstream processing method for producing an antimicrobial peptide, pexiganan, using recombinant Escherichia coli (E. coli). The four helix bundle structure of the unique carrier protein DAMP4 was used to facilitate a simple and cheap purification process based on a selective thermochemical precipitation. Highly pure fusion protein DAMP4-pexiganan was obtained at high yield (around 24 mg per 800 mL cell culture with a final cultivation OD ~ 2). The purification yield of DAMP4-pexiganan protein is increased twofold with a 72.9% of the protein recovery in this study as compared to the previous purification processes (Dwyer in Chem Eng Sci 105:12-21, 2014). The antimicrobial peptide pexiganan was released and activated from the fusion protein by a simple acid-cleavage. Isoelectric precipitation was then applied to separate the pexiganan peptide from the DAMP4 protein carrier. The final yield of pure bio-produced pexiganan was 1.6 mg from 800 mL of bacterial cell culture (final cultivation OD ~ 2). The minimum bactericidal concentration (MBC) test demonstrated that the bio-produced pexiganan has the same antimicrobial activity as chemically synthesized counterpart. This novel downstream process provides a new strategy for simple and probable economic production of antimicrobial peptides.

摘要

抗菌肽(AMPs)作为传统抗生素的替代品具有巨大潜力。然而,目前制备抗菌肽的过程通常繁琐、昂贵且产量低,从而阻碍了它们的研究和应用。迫切需要一种具有成本效益的大规模生产抗菌肽的方法。在本研究中,我们报道了一种可扩展的、无需色谱的下游加工方法,该方法使用重组大肠杆菌(E. coli)生产抗菌肽pexiganan。独特的载体蛋白DAMP4的四螺旋束结构被用于促进基于选择性热化学沉淀的简单且廉价的纯化过程。以高产量获得了高纯度的融合蛋白DAMP4-pexiganan(每800 mL细胞培养物约24 mg,最终培养OD2)。与先前的纯化过程相比,本研究中DAMP4-pexiganan蛋白的纯化产率提高了两倍,蛋白质回收率为72.9%(Dwyer,《化学工程科学》105:12 - 21,2014)。通过简单的酸裂解从融合蛋白中释放并激活抗菌肽pexiganan。然后应用等电沉淀从DAMP4蛋白载体中分离出pexiganan肽。从800 mL细菌细胞培养物(最终培养OD2)中获得的纯生物生产的pexiganan的最终产量为1.6 mg。最低杀菌浓度(MBC)测试表明,生物生产的pexiganan与化学合成的对应物具有相同的抗菌活性。这种新颖的下游工艺为简单且可能经济地生产抗菌肽提供了一种新策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3766/5783979/8939f50d5a6b/13568_2018_541_Fig1_HTML.jpg

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