Viral Vector Vaccine Mfg.
Process Train for Viral Vector Vaccines
A live vector vaccine uses an attenuated or harmless microorganism such as an adenovirus to transport portions of an antigen to stimulate an immune response. Vectored vaccines are capable of inducing potent cell-mediated immunity, which is essential for complex disease like AIDS, malaria, and cancer among others.
While the manufacturing process for vaccine vectors is fairly templated, some challenges may arise, since several different viruses with varying properties can be used. For large viral vectors, process sterility is critical due to yield loss associated with sterile filtration. There are also challenges with vector aggregation and stability.
In addition, many Phase I/II processes involve adherent cell cultures; as a result, scaling to Phase III and commercial manufacturing can require process adjustments to achieve production targets. In later phases, product yield and purity are critical, as high dosage titers are required in the final product. Learn more about viral vector vaccine manufacturing.
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Accelerate Time to Clinical While Ensuring Reliable Scale-up
Upstream culture processes developed for manufacturing of viral vector vaccines must be optimized to meet productivity requirements. This optimization includes the cell lysis and clarification steps which are essential for removal of cells and cell debris and to ensure a robust vector harvest. The upstream process is only successful, however, if it can be reliably scaled in order to meet anticipated market demand.
Achieve Yield and Efficiency Goals with Robust Impurity Removal
Nucleic acids from lysed cells are a common contaminant in viral vector vaccine processes. Regulations require that the level of carry-over host cell nucleic acid be below 10 ng/dose of attenuated viral vaccine. Benzonase® endonuclease treatment followed by tangential flow filtration is a robust and powerful combination to degrade and remove residual nucleic acid components.
Maximize Downstream Recovery
Small-scale clinical lots are typically purified using CsCl-based density gradient ultracentrifugation, while large-scale production requires a two- or three-step chromatography process. Anion exchange is typically used to remove HCP, DNA, RNA, and other major contaminants, while size exclusion chromatography is used for trace contaminant removal.
Ensure Patient Safety
Sterile filtration ensures the sterility of the final formulated product and patient safety. A filter pore size of 0.22 µm or less is required to eliminate microbial contaminants. A key consideration for the sterile filtration process is the level of viral aggregates. These aggregates need to be controlled by optimizing the formulation, otherwise, the sterile filtration process will be challenging with the potential for high losses in yield.
Nuclease Treatment & Clarification
Ensure robust scalability.
- Nuclease Treatment with Benzonase® Suitable for Biopharmaceutical Production EMPROVE® Bio
- Benzonase® Detection with Benzonase® Elisa Kit II to Detect Left Over Benzonase® Endonuclease in the Process
- Primary/Secondary Clarification with Millistak+® HC POD Depth Filters
- Primary Clarification with Clarisolve® Depth Filters
- Clarification Depth Filters & Pretreatment Solutions
- Clarification with Milligard® PES filters
Downstream - Tangential Flow Filtration
Achieve yield, efficiency and pDNA recovery goals while ensuring robust impurity removal.
- Ultrafiltration / Diafiltration with Pellicon® 2 Cassettes
- Ultrafiltration / Diafiltration with Pellicon® 3 Cassettes
- Ultrafiltration / Diafiltration with Pellicon® Capsule with Ultracel® Membrane
- Mobius® TFF 80 System, Mobius® FlexReady Solution for TFF, Cogent® Lab Systems and Cogent® Process-scale Tangential Flow Filtration System
Downstream Chromatography
- Membrane Chromatography with Eshmuno® Q Resin
- Membrane Chromatography with Natrix® Q Recon Mini Chromatography Membranes
- Membrane Chromatography with Natrix® Q Pilot Chromatography Membrane
- Membrane Chromatography with Natrix® Q Recon Mini
- Membrane Chromatography with Eshmuno® Q Resin
- Capture and/or Polishing Chromatography with Fractogel® EMD DEAE Chromatography Resins
- Capture and/or Polishing Chromatography with Fractogel® EMD DMAE Chromatography Resins
- Mobius® FlexReady Solution for Chromatography
Downstream Process Chemicals and Formulation
Bioprocessing Liquid Cell Culture Media & Buffers
We offer the industry’s highest quality sterile filtered liquid capabilities, supplying ready-to-use cell culture media, buffers, CIP and SIP products from GMP facilities worldwide to optimize your biopharma production.
Final Sterile Filtration & Filling
Ensure patient safety with a reliable and robust sterile filtration process.
Analytics Software & PAT Technology
Related Resources
- Application Guide: Biopharmaceutical
A search tool to help you overcome your manufacturing challenges.
- Mini-Handbook: Viral Vector Vaccine Bioprocessing
The manufacturing process for adenovirus vectors is straightforward and fairly templated; a general outline is explained in this handbook.
- White Paper: Developing an Accelerated and More Cost-Effective Single-Use Adenoviral Vector Vaccine Manufacturing Process
Our collaboration with the Jenner Institute has resulted in a single-use, scalable GMP template for manufacture of adenoviral-based vaccines. Learn more on this faster and more cost-effective approach to vaccine manufacturing.
- Application Note: Effect of Benzonase® Endonuclease Addition to Purification of Sabin Polio Virus Type 3
This Application Note summarizes the benefits of incorporating Benzonase® endonuclease in a polio virus type 3 production process.
- Article: Robust Harvest Clarification For Adeno-Associated Viral Vectors Via Depth Filtration
We demonstrate that depth filters clarify AAV vectors, helping to overcome the unique separation challenges presented by these important vectors for gene therapy.
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