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通过合理的代谢途径诱变产生高雷帕霉素产生菌,并通过补料分批生物过程优化进一步提高效价。

Generation of high rapamycin producing strain via rational metabolic pathway-based mutagenesis and further titer improvement with fed-batch bioprocess optimization.

机构信息

Department of Chemical and Biological Engineering, Institute of Biological Engineering, Zhejiang University, Hangzhou 310027, Zhejiang, China.

出版信息

Biotechnol Bioeng. 2010 Oct 15;107(3):506-15. doi: 10.1002/bit.22819.

DOI:10.1002/bit.22819
PMID:20517869
Abstract

Rapamycin is a triene macrolide antibiotic produced by Streptomyces hygroscopicus. Besides its wide application as an effective immunosuppressive agent, other important bioactivities have made rapamycin a potential drug lead for novel pharmaceutical development. However, the low titer of rapamycin in the original producer strain limits further industrialization efforts and restricts its use for other applications. Predicated on knowledge of the metabolic pathways related to rapamycin biosynthesis in S. hygroscopicus, we have rationally designed approaches to generate a rapamycin high producer strain of S. hygroscopicus HD-04-S. These have included alleviation of glucose repression, improved tolerance towards lysine and shikimic acid, and auxotrophy of tryptophan and phenylalanine through the application of stepwise UV mutagenesis. The resultant strain produced rapamycin at 450 mg/L in the shake flask scale. These fermentations were further scaled up in 120 and 20,000 L fermentors, respectively, at the pilot plant. Selected fermentation factors including agitation speed, pH, and on-line supplementation were systematically evaluated. A fed-batch strategy was established to maximize rapamycin production. With these efforts, an optimized fermentation process in the larger scale fermentor was developed. The final titer of rapamycin was 812 mg/L in the 120 L fermentor and 783 mg/L in the 20,000 L fermentor. This work highlights a high rapamycin producing strain derived by mutagenesis and subsequent screening, fermentation optimization of which has now made it feasible to produce rapamycin on an industrial scale by fermentation. The strategies developed here should also be applicable to titer improvement of other important microbial natural products on an industrial scale.

摘要

雷帕霉素是一种由吸水链霉菌产生的三烯大环内酯抗生素。除了作为一种有效的免疫抑制剂被广泛应用外,其其他重要的生物活性使雷帕霉素成为一种有潜力的新药先导化合物,用于新的药物开发。然而,原始生产菌中雷帕霉素的低产量限制了进一步的工业化努力,并限制了其在其他应用中的使用。基于吸水链霉菌中与雷帕霉素生物合成相关的代谢途径的知识,我们已经合理地设计了方法来生成吸水链霉菌 HD-04-S 的雷帕霉素高产菌株。这些方法包括缓解葡萄糖抑制、提高赖氨酸和莽草酸的耐受性,以及通过逐步紫外线诱变使色氨酸和苯丙氨酸成为营养缺陷型。所得菌株在摇瓶规模下产生 450mg/L 的雷帕霉素。这些发酵分别在中试工厂的 120L 和 20000L 发酵罐中进一步放大。系统评估了选定的发酵因素,包括搅拌速度、pH 值和在线补料。建立了分批补料策略以最大化雷帕霉素的产量。通过这些努力,在较大规模的发酵罐中开发了优化的发酵工艺。在 120L 发酵罐中的雷帕霉素最终产量为 812mg/L,在 20000L 发酵罐中的产量为 783mg/L。这项工作突出了通过诱变和随后的筛选得到的高产雷帕霉素菌株,其发酵优化使得通过发酵在工业规模上生产雷帕霉素成为可行。这里开发的策略也应该适用于其他重要微生物天然产物在工业规模上的产量提高。

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