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优化CHO表达平台的战略部署,以推出辉瑞的单克隆抗体产品组合。

Strategic deployment of CHO expression platforms to deliver Pfizer's Monoclonal Antibody Portfolio.

作者信息

Scarcelli John J, Shang Tanya Q, Iskra Tim, Allen Martin J, Zhang Lin

机构信息

Cell Line Development, Biotherapeutics Pharmaceutical Sciences, Pfizer Inc., Andover, MA, 01810.

Analytical Research and Development, Biotherapeutics Pharmaceutical Sciences, Pfizer Inc., Andover, MA, 01810.

出版信息

Biotechnol Prog. 2017 Nov;33(6):1463-1467. doi: 10.1002/btpr.2493. Epub 2017 Jun 2.

Abstract

Development of stable cell lines for expression of large-molecule therapeutics represents a significant portion of the time and effort required to advance a molecule to enabling regulatory toxicology studies and clinical evaluation. Our development strategy employs two different approaches for cell line development based on the needs of a particular project: a random integration approach for projects where high-level expression is critical, and a site-specific integration approach for projects in which speed and reduced employee time spend is a necessity. Here we describe both our random integration and site-specific integration platforms and their applications in support of monoclonal antibody development and production. We also compare product quality attributes of monoclonal antibodies produced with a nonclonal cell pool or clonal cell lines derived from the two platforms. Our data suggests that material source (pools vs. clones) does not significantly alter the examined product quality attributes. Our current practice is to leverage this observation with our site-specific integration platform, where material generated from cell pools is used for an early molecular assessment of a given candidate to make informed decisions around development strategy. © 2017 American Institute of Chemical Engineers Biotechnol. Prog., 33:1463-1467, 2017.

摘要

开发用于表达大分子治疗药物的稳定细胞系,在将一种分子推进到进行监管毒理学研究和临床评估所需的时间和精力中占很大一部分。我们的开发策略根据特定项目的需求采用两种不同的细胞系开发方法:对于高水平表达至关重要的项目采用随机整合方法,对于速度和减少员工时间投入必不可少的项目采用位点特异性整合方法。在此,我们描述了我们的随机整合和位点特异性整合平台及其在支持单克隆抗体开发和生产中的应用。我们还比较了用非克隆细胞库或源自这两个平台的克隆细胞系生产的单克隆抗体的产品质量属性。我们的数据表明,材料来源(细胞库与克隆)不会显著改变所检测的产品质量属性。我们目前的做法是将这一观察结果与我们的位点特异性整合平台相结合,在该平台中,从细胞库产生的材料用于对给定候选物进行早期分子评估,以便围绕开发策略做出明智的决策。© 2017美国化学工程师学会生物技术进展,33:1463 - 1467,2017年。

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