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Process characterization strategy for a precipitation step for host cell protein reduction

机译:宿主细胞蛋白减少沉淀步骤的过程表征策略

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Process characterization using QbD approaches has rarely been described for precipitation steps used for impurity removal in biopharmaceutical processes. We propose a two-step approach for process characterization in which the first step focuses on product quality and the second focuses on process performance. This approach provides an efficient, streamlined strategy for the characterization of precipitation steps under the Quality by Design paradigm. This strategy is demonstrated by a case study for the characterization of a precipitation using sodium caprylate to reduce host cell proteins (HCP) during a monoclonal antibody purification process. Process parameters were methodically selected through a risk assessment based on prior development data and scientific knowledge described in the literature. The characterization studies used two multivariate blocks to decouple and distinguish the impact of product quality (e.g., measured HCP of the recovered product from the precipitation) and process performance (e.g., step yield). Robustness of the precipitation step was further demonstrated through linkage studies across the overall purification process. HCP levels could be robustly reduced to <= 100 ppm in the drug substance when the precipitation step operated within an operation space of <= 1% (m/v) sodium caprylate, pH 5.0-6.0, and filter flux <= 300 L/m(2)-hr for a load HCP concentration up to 19,000 ppm. This two-step approach for characterization of precipitation steps has several advantages, including tailoring of the experimental design and scale-down model to the intended purpose for each step, use of a manageable number of experiments without compromising scientific understanding, and limited time and material consumption.
机译:使用QBD方法的方法表征很少用于用于在生物制药过程中除去杂质去除的沉淀步骤。我们提出了一种用于过程表征的两步方法,其中第一步侧重于产品质量,第二步专注于过程性能。这种方法提供了一种有效的流线型策略,用于通过设计范式来表征质量下的降水步骤。通过壳体研究证明了使用辛酸钠沉淀的沉淀来证明该策略,以在单克隆抗体纯化过程中减少宿主细胞蛋白(HCP)。通过基于文献中描述的先前开发数据和科学知识的风险评估,通过风险评估有条理地选择过程参数。表征研究使用了两种多变量块来分离并区分产品质量的影响(例如,从沉淀的回收产物的测量HCP)和工艺性能(例如,步骤产量)。通过整体纯化过程的连杆研究进一步证明了沉淀步骤的鲁棒性。当在沉淀步骤在<= 1%(m / v)辛酸盐,pH5.0-6.0和过滤磁通量<= 300L / M(2)-HR负载HCP浓度高达19,000ppm。这种两步方法,用于沉淀步骤的表征具有几个优点,包括剪裁实验设计和缩小模型的预期目的,用于每一步的预期目的,使用管理数量的实验,而不会影响科学的理解,以及有限的时间和材料消耗。

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