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通过无线控制补料分批系统在摇瓶中提高毕赤酵母中人类II型原胶原蛋白的产量。

Improved production of human type II procollagen in the yeast Pichia pastoris in shake flasks by a wireless-controlled fed-batch system.

作者信息

Ruottinen Maria, Bollok Monika, Kögler Martin, Neubauer Antje, Krause Mirja, Hämäläinen Eija-Riitta, Myllyharju Johanna, Vasala Antti, Neubauer Peter

机构信息

Bioprocess Engineering Laboratory, Dept, of Process and Environmental Engineering, University of Oulu, P.O. Box 4300, FIN-90014 University of Oulu, Finland.

出版信息

BMC Biotechnol. 2008 Mar 27;8:33. doi: 10.1186/1472-6750-8-33.

Abstract

BACKGROUND

Here we describe a new technical solution for optimization of Pichia pastoris shake flask cultures with the example of production of stable human type II collagen. Production of recombinant proteins in P. pastoris is usually performed by controlling gene expression with the strong AOX1 promoter, which is induced by addition of methanol. Optimization of processes using the AOX1 promoter in P. pastoris is generally done in bioreactors by fed-batch fermentation with a controlled continuous addition of methanol for avoiding methanol toxification and carbon/energy starvation. The development of feeding protocols and the study of AOX1-controlled recombinant protein production have been largely made in shake flasks, although shake flasks have very limited possibilities for measurement and control.

RESULTS

By applying on-line pO2 monitoring we demonstrate that the widely used pulse feeding of methanol results in long phases of methanol exhaustion and consequently low expression of AOX1 controlled genes. Furthermore, we provide a solution to apply the fed-batch strategy in shake flasks. The presented solution applies a wireless feeding unit which can be flexibly positioned and allows the use of computer-controlled feeding profiles. By using the human collagen II as an example we show that a quasi-continuous feeding profile, being the simplest way of a fed-batch fermentation, results in a higher production level of human collagen II. Moreover, the product has a higher proteolytic stability compared to control cultures due to the increased expression of human collagen prolyl 4-hydroxylase as monitored by mRNA and protein levels.

CONCLUSION

The recommended standard protocol for methanol addition in shake flasks using pulse feeding is non-optimal and leads to repeated long phases of methanol starvation. The problem can be solved by applying the fed-batch technology. The presented wireless feeding unit, together with an on-line monitoring system offers a flexible, simple, and low-cost solution for initial optimization of the production in shake flasks which can be performed in parallel. By this way the fed-batch strategy can be applied from the early screening steps also in laboratories which do not have access to high-cost and complicated bioreactor systems.

摘要

背景

在此,我们以稳定型人II型胶原蛋白的生产为例,描述一种优化毕赤酵母摇瓶培养的新技术方案。在毕赤酵母中生产重组蛋白通常通过用强AOX1启动子控制基因表达来实现,该启动子由添加甲醇诱导。在毕赤酵母中使用AOX1启动子的工艺优化一般在生物反应器中通过补料分批发酵进行,即控制连续添加甲醇以避免甲醇中毒和碳/能量饥饿。尽管摇瓶在测量和控制方面的可能性非常有限,但补料方案的开发以及AOX1控制的重组蛋白生产的研究大多在摇瓶中进行。

结果

通过应用在线pO2监测,我们证明广泛使用的甲醇脉冲补料会导致甲醇耗尽的长时间阶段,从而导致AOX1控制基因的低表达。此外,我们提供了一种在摇瓶中应用补料分批策略的解决方案。所提出的解决方案应用了一种无线补料单元,该单元可以灵活定位,并允许使用计算机控制的补料曲线。以人胶原蛋白II为例,我们表明准连续补料曲线作为补料分批发酵最简单的方式,可导致人胶原蛋白II的更高生产水平。此外,与对照培养物相比,由于通过mRNA和蛋白质水平监测到人胶原蛋白脯氨酰4-羟化酶的表达增加,该产品具有更高的蛋白水解稳定性。

结论

在摇瓶中使用脉冲补料添加甲醇的推荐标准方案并非最优,会导致甲醇饥饿的反复长时间阶段。该问题可以通过应用补料分批技术来解决。所提出的无线补料单元与在线监测系统一起,为摇瓶中生产的初始优化提供了一种灵活、简单且低成本的解决方案,可并行进行。通过这种方式,补料分批策略也可以从早期筛选步骤开始应用于没有高成本和复杂生物反应器系统的实验室。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/532b/2315644/f14fd337e075/1472-6750-8-33-1.jpg

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