Biosimilars: SOP for Fed-Batch Cultivation Strategy in Bioreactor Operations – V 2.0
Standard Operating Procedure for Fed-Batch Cultivation Strategy in Bioreactor Operations for Biosimilars
Department |
Biosimilars |
SOP No. |
SOP/BS/074/2025 |
Supersedes |
SOP/BS/074/2022 |
Page No. |
Page 1 of 13 |
Issue Date |
04/05/2025 |
Effective Date |
06/05/2025 |
Review Date |
04/05/2026 |
1. Purpose
To define the process for executing fed-batch cultivation in bioreactor operations for biosimilar production, ensuring consistent cell growth, product yield, and regulatory compliance under GMP conditions.
2. Scope
This SOP applies to all fed-batch bioreactor campaigns used in mammalian cell culture for biosimilar manufacturing within the upstream processing department.
3. Responsibilities
- Bioprocess Operators: Execute feed protocols, monitor parameters, and document observations.
- Process Engineers: Design feed strategies and adjust based on culture performance.
- QA Personnel: Verify adherence to batch instructions and review feed records.
4. Accountability
The Head of Upstream Processing is accountable for ensuring fed-batch protocols are implemented as per validated procedures and deviations are managed appropriately.
5. Procedure
5.1 Pre-Cultivation Preparation
- Ensure the bioreactor is pre-calibrated and sterile.
- Prepare feed solutions (e.g., glucose, amino acids, lipids) as per formulation guidelines. Filter sterilize and store under refrigerated conditions.
- Verify feed volumes and label feed vessels with batch number and composition (Annexure-1).
5.2 Inoculation and Batch Phase
- Inoculate culture at 0.3–0.5 × 106 cells/mL and monitor growth for 24–48 hours.
- Maintain temperature, pH, DO, and agitation as per the master batch record.
5.3 Feed Initiation
- Begin feeding once VCD reaches 1.0–1.5 × 106 cells/mL or glucose falls below 2 g/L.
- Start initial bolus feed of glucose (2%–4% final concentration) using sterile tubing or pump.
5.4 Continuous Feed Strategy
- Implement feed as per predetermined schedule:
- Fixed volume daily (e.g., 10 mL/L)
- OR exponential feeding based on cell growth and metabolic needs
- Monitor glucose, lactate, and ammonia levels every 12 hours.
- Adjust feed concentration or timing based on nutrient consumption.
5.5 DO and pH Integration
- Link DO feedback to agitation and oxygen cascade.
- Ensure feed does not result in drastic pH drift; adjust with buffers or antifoam agents as necessary.
5.6 End of Cultivation
- Stop feeding when VCD plateaus or viability drops below 80%.
- Record total feed volume and culture parameters (Annexure-2).
- Proceed to harvest as per SOP/BS/086/2025.
6. Abbreviations
- VCD: Viable Cell Density
- DO: Dissolved Oxygen
- GMP: Good Manufacturing Practice
7. Documents
- Feed Solution Label – Annexure-1
- Feed Monitoring Log – Annexure-2
8. References
- ICH Q8 – Pharmaceutical Development
- WHO TRS 999 – Guidelines for Biopharmaceutical Production
- SOP/BS/086/2025 – Harvest Process
9. SOP Version
Version: 2.0
10. Approval Section
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Prepared By |
Checked By |
Approved By |
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11. Annexures
Annexure-1: Feed Solution Label
Feed Type |
Composition |
Volume |
Batch No. |
Prepared By |
Date |
Feed A |
Glucose 40%, Amino Acids |
2L |
FB-074-A |
Rajesh Kumar |
04/05/2025 |
Annexure-2: Feed Monitoring Log
Date |
Time |
Feed Volume (mL) |
Glucose (g/L) |
Lactate (mM) |
Remarks |
04/05/2025 |
12:00 |
100 |
2.1 |
1.8 |
Normal |
Revision History:
Revision Date |
Revision No. |
Revision Details |
Reason for Revision |
Approved By |
04/05/2025 |
2.0 |
Expanded section on exponential feeding and integrated DO/pH control |
Process Optimization |
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