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碳代谢限制毕赤酵母中重组蛋白的生产。

Carbon metabolism limits recombinant protein production in Pichia pastoris.

机构信息

Department of Biochemical and Chemical Engineering, Laboratory of Chemical Biotechnology, TU Dortmund University, Emil-Figge-Str 66, D-44227 Dortmund, Germany.

出版信息

Biotechnol Bioeng. 2011 Aug;108(8):1942-53. doi: 10.1002/bit.23114. Epub 2011 Mar 11.

Abstract

The yeast Pichia pastoris enables efficient (high titer) recombinant protein production. As the molecular tools required are well established and gene specific optimizations of transcription and translation are becoming available, metabolism moves into focus as possible limiting factor of recombinant protein production in P. pastoris. To investigate the impact of recombinant protein production on metabolism systematically, we constructed strains that produced the model protein β-aminopeptidase BapA of Sphingosinicella xenopeptidilytica at different production yields. The impact of low to high BapA production on cell physiology was quantified. The data suggest that P. pastoris compensates for the additional resources required for recombinant protein synthesis by reducing by-product formation and by increasing energy generation via the TCA cycle. Notably, the activity of the TCA cycle was constant with a rate of 2.1 ± 0.1 mmol g CDW-1 h(-1) irrespective of significantly reduced growth rates in high BapA producing strains, suggesting an upper limit of TCA cycle activity. The reduced growth rate could partially be restored by providing all 20 proteinogenic amino acids in the fermentation medium. Under these conditions, the rate of BapA synthesis increased twofold. The successful supplementation of the growth medium by amino acids to unburden cellular metabolism during recombinant protein production suggests that the metabolic network is a valid target for future optimization of protein production by P. pastoris.

摘要

酵母毕赤酵母能够高效(高滴度)生产重组蛋白。由于所需的分子工具已经成熟,并且转录和翻译的基因特异性优化也变得可行,因此代谢成为毕赤酵母中重组蛋白生产的可能限制因素。为了系统地研究重组蛋白生产对代谢的影响,我们构建了在不同生产产量下生产模式蛋白β-氨基肽酶 BapA 的毕赤酵母菌株。定量研究了低至高 BapA 产量对细胞生理学的影响。数据表明,毕赤酵母通过减少副产物的形成和通过增加 TCA 循环来增加能量生成来补偿重组蛋白合成所需的额外资源。值得注意的是,TCA 循环的活性保持不变,其速率为 2.1 ± 0.1 mmol g CDW-1 h-1,而在高 BapA 产生菌株中生长速率显著降低,表明 TCA 循环活性存在上限。通过在发酵培养基中提供所有 20 种蛋白质氨基酸,可以部分恢复降低的生长速率。在这些条件下,BapA 合成的速率增加了两倍。在重组蛋白生产过程中通过向生长培养基中添加氨基酸来减轻细胞代谢负担的成功补充表明,代谢网络是未来优化毕赤酵母蛋白生产的有效目标。

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