Abstract
Reliable process development is accompanied by intense experimental effort. The utilization of an intensified design of experiments (iDoE) (intra-experimental critical process parameter (CPP) shifts combined) with hybrid modeling potentially reduces process development burden. The iDoE can provide more process response information in less overall process time, whereas hybrid modeling serves as a commodity to describe this behavior the best way. Therefore, a combination of both approaches appears beneficial for faster design screening and is especially of interest at larger scales where the costs per experiment rise significantly. Ideally, profound process knowledge is gathered at a small scale and only complemented with few validation experiments on a larger scale, saving valuable resources. In this work, the transferability of hybrid modeling for Chinese hamster ovary cell bioprocess development along process scales was investigated. A two-dimensional DoE was fully characterized in shake flask duplicates (300 ml), containing three different levels for the cultivation temperature and the glucose concentration in the feed. Based on these data, a hybrid model was developed, and its performance was assessed by estimating the viable cell concentration and product titer in 15 L bioprocesses with the same DoE settings. To challenge the modeling approach, 15 L bioprocesses also comprised iDoE runs with intra-experimental CPP shifts, impacting specific cell rates such as growth, consumption, and formation. Subsequently, the applicability of the iDoE cultivations to estimate static cultivations was also investigated. The shaker-scale hybrid model proved suitable for application to a 15 L scale (1:50), estimating the viable cell concentration and the product titer with an NRMSE of 10.92% and 17.79%, respectively. Additionally, the iDoE hybrid model performed comparably, displaying NRMSE values of 13.75% and 21.13%. The low errors when transferring the models from shaker to reactor and between the DoE and the iDoE approach highlight the suitability of hybrid modeling for mammalian cell culture bioprocess development and the potential of iDoE to accelerate process characterization and to improve process understanding.
Highlights
Tremendous effort is spent performing design of experiments (DoE) as part of process characterization and optimization (Hakemeyer et al, 2016; Tripathi and Shrivastava, 2019; Bayer et al, 2020b) at different scales
The bolus-fed shake flask cultivations were terminated after 11 days, as the cell viability fell below the threshold
We could show that the information content from intensified design of experiments (iDoE) experiments in the 15 L scale is comparable to that from DoE experiments
Summary
Tremendous effort is spent performing design of experiments (DoE) as part of process characterization and optimization (Hakemeyer et al, 2016; Tripathi and Shrivastava, 2019; Bayer et al, 2020b) at different scales. This leads to a huge burden on process development and enormous consumption of resources. Several factors, referred to as critical process parameters (CPPs), can have an impact on the produced quantity of the target molecule and certain critical quality attributes (CQAs) This impact is either directly due to changes in the surrounding environment or indirectly due to altering how cells are producing the target molecules
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