Tim Tressel scite author profile

The large-scale production of recombinant human monoclonal antibodies demands economical purification processes with high throughputs. In this article we briefly describe a common antibody process and evaluate the Q membrane adsorber for process-scale antibody production as an alternative to a Q-packed-bed column in a flow-through mode. The scientific concepts underlining Q membrane technology and its application are reviewed. The disadvantages and advantages of using Q membrane chromatography as a purification unit in large-scale production are discussed, including problems initially seen with the Q membrane scale-down model but solved with the invention of a new scale-down model. The new Q-membrane unit operation has a process capacity greater than 3,000 g/m(2) or 10.7 kg/L with a LRV over 5 for four model viruses. In this Review, a cost analysis illustrates that Q membrane chromatography is a viable alternative to Q column chromatography as a polishing step in a flow-through mode for process-scale antibody production.

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New Q membrane scale-down model for process-scale antibody purification

Zhou

Tressel

Gottschalk

et al. 2006

Journal of Chromatography A

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Current Therapeutic Antibody Production and Process Optimization

Feng¹,

Lee²,

Zhou³

et al. 2006

BioProcess J

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Viral clearance using disposable systems in monoclonal antibody commercial downstream processing

Zhou

Solamo

Hong

et al. 2008

Biotech & Bioengineering

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Once highly selective protein A affinity is chosen for robust mAb downstream processing, the major role of polishing steps is to remove product related impurities, trace amounts of host cell proteins, DNA/RNA, and potential viral contaminants. Disposable systems can act as powerful options either to replace or in addition to polishing column chromatography to ensure product purity and excellent viral clearance power for patients' safety. In this presentation, the implementation of three disposable systems such as depth filtration, membrane chromatography, and nanometer filtration technology in a commercial process are introduced. The data set of viral clearance with these systems is presented. Application advantages and disadvantages including cost analysis are further discussed.

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Tim Tressel

Downstream processing of monoclonal antibodies—Application of platform approaches

Basic Concepts in Q Membrane Chromatography for Large-Scale Antibody Production

New Q membrane scale-down model for process-scale antibody purification

Current Therapeutic Antibody Production and Process Optimization

Viral clearance using disposable systems in monoclonal antibody commercial downstream processing

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