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采用微孔过滤逆流洗涤连续沉淀单克隆抗体。

Continuous precipitation for monoclonal antibody capture using countercurrent washing by microfiltration.

机构信息

Department of Chemical Engineering, The Pennsylvania State University, Pennsylvania.

Department of Chemical Engineering, Carnegie Mellon University, Pittsburgh, Pennsylvania.

出版信息

Biotechnol Prog. 2019 Nov;35(6):e2886. doi: 10.1002/btpr.2886. Epub 2019 Aug 8.

Abstract

There is renewed interest in the possibility of using precipitation for initial capture of high-value therapeutic proteins as part of an integrated continuous downstream process. Precipitation is greatly facilitated by the high product titers now achieved in most cell culture processes, in sharp contrast to chromatographic processes whose performance is reduced at high titers. The current study used a combination of reversible cross-linking (zinc chloride, ZnCl ) and volume exclusion (polyethylene glycol) agents to precipitate a monoclonal antibody product directly from harvested cell culture fluid using a continuous tubular precipitation reactor. The precipitates were then dewatered and continuously washed using tangential flow filtration, with a countercurrent-staged configuration used to reduce the amount of wash buffer required and increase host cell protein removal. Long-term operation was achieved by operating the membrane modules below the critical filtrate flux to avoid fouling. Experimental results demonstrate the feasibility of this fully continuous integrated precipitation process at bench scale, with design calculations used to explore the key factors affecting the performance of this system for initial antibody capture.

摘要

人们重新产生了兴趣,希望能够利用沉淀作用来初步捕获高价值的治疗性蛋白质,将其作为集成式连续下游工艺的一部分。由于现在在大多数细胞培养过程中都能实现很高的产物滴度,沉淀作用变得更加容易,这与色谱过程形成鲜明对比,色谱过程在高滴度下的性能会降低。本研究使用可逆交联(氯化锌,ZnCl )和体积排阻剂的组合,直接从收获的细胞培养液中使用连续管状沉淀反应器沉淀单克隆抗体产物。然后使用切向流过滤对沉淀物进行脱水和连续洗涤,采用逆流分阶段配置以减少所需洗涤缓冲液的量并提高宿主细胞蛋白去除率。通过在临界过滤通量以下操作膜组件来避免堵塞,从而实现长期运行。实验结果证明了在台架规模下全连续集成沉淀工艺的可行性,并使用设计计算来探讨影响该系统初始抗体捕获性能的关键因素。

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