mAb Downstream Processing

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Enhance productivity in downstream processing

As upstream work drives higher monoclonal antibody (mAb) titers, downstream teams face greater pressure to maintain recovery while reducing impurities, such as aggregates, host cell proteins (HCPs), and residual DNA. Defining resin-buffer conditions early helps manage these shifts in load and impurity profiles. Applying high-throughput screening (HTS) tools with MabCaptureC Protein A (ProA) chromatography resin and POROS resins, supported by structured buffer options, enables more reliable capture and polish development. Teams may also benefit from Field Application Scientist (FAS) support when interpreting screening results.

Workflow-based mAb upstream development strategies


Gain practical guidance on improving processes by exploring strategies for cell line selection, media and feed screening, and early bioreactor optimization in this webinar summary.
 

Streamline mAb downstream process development

Finding suitable purification conditions for mAbs can take significant time, especially when load characteristics and impurity profiles shift with upstream changes. Incorporating structured resin and buffer screening early helps narrow viable options more efficiently. HTS formats support fast evaluation of bind, wash, and elute conditions, enabling teams to define capture and polish strategies with greater confidence.

Refine resin-buffer selection with high-throughput screening

Evaluate resin-buffer combinations efficiently using tools, such as the Resin Selection Tool, 96-well screening plates, RoboColumn™ formats, and pre-packed columns, designed to compare bind-and-elute behaviors across conditions.

 

Efficient mAb manufacturing with Protein A resin

Improve mAb downstream processing by applying MabCaptureC ProA resin during capture. It is designed with manufacturing cost-savings in mind, and with high binding capacity and alkaline stability to support consistent purification performance.


Refine polish steps with POROS resins

Address mAb polish challenges by applying POROS anion exchange chromatography (AEX), cation exchange chromatography (CEX), and hydrophobic interaction chromatography (HIC) resins, as well as mixed-mode resin. Target aggregates, charge variants, HCPs, and residual DNA using selection tools.

Apply subdomain-specific affinity chromatography

Adapt capture strategies when evolving antibody formats and impurity profiles challenge standard approaches. Subdomain-specific affinity resins can introduce greater selectivity earlier in downstream workflows. This targeted capture can help reduce reliance on additional polishing steps and support a more controlled purification design for complex mAb programs.
 

Maintain quality with analytical and impurity testing tools


Empower the downstream processing (DSP) of mAbs by applying analytical methods that help monitor purity, quantify impurities, and track process consistency as conditions evolve. Use residual Chinese hamster ovary (CHO) DNA detection, HCP analysis, and identity and purity assays to help confirm clearance during capture and polish steps. These tools support process needs and help maintain product quality as mAb workflows advance.

Explore the 3D mAb workflow

Frequently asked questions

Choosing resin and buffer conditions means matching resin chemistry with shifting load and impurity profiles. Using 96-well screening plates, POROS resins, and buffer libraries, teams can rapidly identify optimal combinations for recovery and purity across capture and polish steps. FAS support can help guide the interpretation of screening data.

High-throughput screening in mAb DSP typically uses resin slurry plates or mini-column formats. Resin slurry plates enable broad condition testing with low capital needs and flexible operating ranges, making them well-suited for early scouting. Mini-columns, including pre-packed formats, offer more representative chromatography behavior and support detailed comparison of resin performance under defined process conditions.

Improving mAb recovery during capture requires balancing binding capacity with conditions that promote selective elution of impurities. MabCaptureC resin supports this balance through its high dynamic binding capacity and robust, alkaline-tolerant ligand. Pairing the resin with structured buffer optimization, such as evaluating pH, conductivity, and wash conditions, helps refine recovery while maintaining effective reduction of HCPs, aggregates, and other early-stage contaminants.

Scaling mAb purification requires confirming that resin performance, buffer use, and chromatographic behavior remain predictable as column dimensions and equipment change. Screening plates and small pre-packed columns help define conditions that translate reliably to larger formats. POROS resins, designed for consistent mass transfer across scales, support a smooth transition from development studies to clinical or commercial manufacturing.

High-titer feeds can increase aggregates, charge variants, HCPs, and residual DNA, placing more pressure on polish operations. Using AEX, CEX, ion exchange chromatography (IEX), and HIC resins allow targeted reduction of these species under defined pH and conductivity ranges. The Resin Selection Tool helps match resin chemistry with impurity profiles, supporting efficient reduction strategies as conditions scale or shift.

There are generally two instances where non-ProA affinity resins targeting other antibody subdomains are worth evaluating. Sometimes the structure of non-traditional antibody-based therapeutics, such as bispecifics and Fab fragments, has altered ProA binding sites and recovery can be an issue, or using different affinity resins can offer enhanced selectivity between target and misformed pairs or aggregates. In addition, feedstreams of these advanced modalities are often more complex than those of traditional mAbs, containing more difficult to remove impurities. Employing different affinity resins at the capture step can help reduce the product-related impurity burden on subsequent steps.

Supporting other therapeutic antibody development

Thermo Fisher also supports the development and manufacturing of additional therapeutic antibody modalities, including antibody-drug conjugates (ADCs) and bispecific antibodies (bsAbs). Explore these modalities within the broader bioprocessing applications framework.

Antibody-drug conjugates (ADCs)

Support ADC development with solutions built to streamline antibody production, conjugation-ready purification, and analytical workflows that help maintain product quality.
 

Bispecific antibodies (BsAbs)

Advance bsAb development with solutions that support complex molecule expression, purification strategies that manage chain pairing, and analytical tools that help evaluate product quality and consistency.

For research use or further manufacturing. Not for diagnostic use or direct administration into humans or animals.