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Rationale-based selection of optimal operating strategies and gene dosage impact on recombinant protein production in Komagataella phaffii (Pichia pastoris)

机译:基于理性的优化经营策略和基因剂量对Komagataella Phaffii(Pichia Pastoris)的重组蛋白质产生的影响选择

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摘要

Its features as a microbial and eukaryotic organism have turned Komagataella phaffii (Pichia pastoris) into an emerging cell factory for recombinant protein production (RPP). As a key step of the bioprocess development, this work aimed to demonstrate the importance of tailor designing the cultivation strategy according to the production kinetics of the cell factory. For this purpose, K. phaffii clones constitutively expressing (P-GAP) Candida rugosa lipase 1 (Crl1) with different gene dosage were used as models in continuous and fed-batch cultures. Production parameters were much greater with a multicopy clone (MCC) than with the single-copy clone (SCC). Regarding production kinetics, the specific product generation rate (q(P)) increased linearly with increasing specific growth rate (mu) in SCC; by contrast, q(P) exhibited saturation in MCC. A transcriptional analysis in chemostat cultures suggested the presence of eventual post-transcriptional bottlenecks in MCC. After the strain characterization, in order to fulfil overall development of the bioprocess, the performance of both clones was also evaluated in fed-batch mode. Strikingly, different optimal strategies were determined for both models due to the different production kinetic patterns observed as a trade-off for product titre, yields and productivity. The combined effect of gene dosage and adequate mu enables rational process development with a view to optimize K. phaffii RPP bioprocesses.
机译:其作为微生物和真核生物的特征使Komagataella Phaffii(Pichia Pastoris)转变为一个新兴的细胞工厂,用于重组蛋白质生产(RPP)。作为生物过程开发的关键步骤,这项工作旨在展示根据细胞厂的生产动力学裁定设计培养策略的重要性。为此目的,具有不同基因剂量的组成型表达(P-Gap)Candida Rugosa脂肪酶1(CRL1)的K.Phaffii克隆用作连续和补料分批培养物中的模型。通过与单拷贝克隆(SCC)进行多拷贝克隆(MCC),生产参数大大。关于生产动力学,特异性产物产生率(Q(P))随着SCC中增加的特异性生长速率(MU)增加而升高;相比之下,Q(P)在MCC中表现出饱和度。化学蹄类培养物的转录分析表明MCC中的最终转录后瓶颈存在。在应变表征之后,为了满足生物过程的整体发展,还在FED批处理模式下评估了两种克隆的性能。引人注目地,由于产品滴度,产量和生产率的折衷所观察到的不同生产动力学模式,两种模型都确定了不同的最佳策略。基因剂量和足够亩的组合效应使得合理的过程开发能够优化K.Phaffii RPP生物处理。

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