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运用质量源于设计原则,优化单克隆抗体生产工艺,提升稳健性和产品质量。

Optimization of a mAb production process with regard to robustness and product quality using quality by design principles.

作者信息

Wohlenberg Ole Jacob, Kortmann Carlotta, Meyer Katharina V, Schellenberg Jana, Dahlmann Katharina, Bahnemann Janina, Scheper Thomas, Solle Dörte

机构信息

Institut für Technische Chemie Leibniz Universität Hannover Hannover Germany.

出版信息

Eng Life Sci. 2022 Jun 3;22(7):484-494. doi: 10.1002/elsc.202100172. eCollection 2022 Jul.

Abstract

Quality by Design principles are well described and widely used in biopharmaceutical industry. The characterization of a monoclonal antibody (mAb) production process is crucial for novel process development and control. Yet, the application throughout the entire upstream process was rarely demonstrated. Following previously published research, this study marks the second step toward a complete process characterization and is focused on the effect of critical process parameters on the antibody production efficiency and quality of the process. In order to conduct the complex Design of Experiments approach with optimal control and comparability, the ambr®15 micro bioreactor platform was used. Investigated parameters included the pH and dissolved oxygen set points, the initial viable cell density (iVCD) as well as the N-1 duration. Various quality attributes (e.g., growth rate, viability, mAb titer, and peak proportion) were monitored and analyzed using multivariate data analysis to evaluate the parameter effects. The pH set point and the initial VCD were identified as key process parameters with strong influence on the cell growth as well as the mAb production and its proportion to the total protein concentration. For optimization and improvement in robustness of these quality attributes the pH must be increased to 7.2, while the iVCD must be lowered to 0.2 × 10 cells/mL. Based on the defined design space, additional experiments verified the results and confirmed the intact bioactivity of the antibody. Thereby, process control strategies could be tuned toward high cell maintenance and mAb production, which enable optimal downstream processing.

摘要

质量源于设计原则在生物制药行业中已有详尽描述并被广泛应用。单克隆抗体(mAb)生产工艺的特性描述对于新工艺的开发和控制至关重要。然而,其在整个上游工艺中的应用却鲜有展示。继先前发表的研究之后,本研究标志着迈向完整工艺特性描述的第二步,重点关注关键工艺参数对抗体生产效率和工艺质量的影响。为了以最佳控制和可比性进行复杂的实验设计方法,使用了ambr®15微型生物反应器平台。研究的参数包括pH值和溶解氧设定点、初始活细胞密度(iVCD)以及N - 1持续时间。使用多变量数据分析监测和分析各种质量属性(例如,生长速率、活力、mAb滴度和峰值比例)以评估参数影响。pH设定点和初始VCD被确定为对细胞生长以及mAb生产及其与总蛋白浓度的比例有强烈影响的关键工艺参数。为了优化和提高这些质量属性的稳健性,pH值必须提高到7.2,而iVCD必须降低到0.2×10细胞/mL。基于定义的设计空间,额外的实验验证了结果并确认了抗体完整的生物活性。由此,工艺控制策略可以朝着高细胞维持和mAb生产进行调整,从而实现最佳的下游加工。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c270/9288990/63913249dfcb/ELSC-22-484-g006.jpg

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