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

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Resumen

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 ) 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 ) increased linearly with increasing specific growth rate (µ) in SCC; by contrast, q 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 µ enables rational process development with a view to optimize K. phaffii RPP bioprocesses. The combined effect of strain and bioprocess engineering should be considered during a rational process development towards bioprocess optimization. The synergy between gene dosage and specific growth rate have been evaluated for the Komagataella phaffii (Pichia pastoris) recombinant protein production (RPP) of an industrial lipase in chemostat and fed-batch cultures. Different optimal strategies were designed from a trade-off for product titer, yields and productivity for two clone models with different gene dosage and production kinetics, from which further transcription analysis supported potential bottlenecks after transcription.
Idioma originalInglés
Páginas (desde-hasta)315-327
Número de páginas13
PublicaciónMicrobial Biotechnology
Volumen13
N.º2
DOI
EstadoPublicada - 2020

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