Achieving High-Throughput CE-SDS While Preserving Data Integrity

Biopharma – protein therapeutics | Analytical Development | PA800 Plus system | BioPhase 8800 system Case study Need: The Analytical Development lab at Teva required a higher throughput CE solution to support stability testing, process development, formulation, and DOE studies forBio CMC programs at Teva Pharmaceuticals. Challenge: Current SOPs in pre-commercial programs utilize the PA 800 Plus system. All data generated using new analytical technologies must produce equivalent data to ensure data continuity from Analytical Development to Quality Control groups. Goal: Develop a system suitability assessment for the BioPhase 8800 system for CGE at Teva Pharmaceuticals to demonstrate data equivalence to the PA 800 Plus system. Impact: Achieve faster data collection and higher throughput while maintaining existing SOPs, enabling the reduction of overall costs and the need for multiple CE instruments. Demonstrating equivalence allows for this method to potentially be applied to commercial and precommercial programs alike. Gaining high throughput without compromising data quality Analytical Development R&D CMC Biologics – Teva Pharmaceuticals Matthew Myers Associate Director - Analytical Development. Teva Pharmaceuticals Current SOPs at Teva for several programs include the use of the PA 800 Plus system for the reduced and non-reduced CE-SDS analysis of antibodies. However, with the number of samples, and programs increasing, the throughput in analytical development needed to increase. This case study discusses the considerations when moving from the PA 800 Plus system to the BioPhase 8800 system in development labs while ensuring method transfer to QC labs. It also showcases how the Teva team plans to implement the BioPhase 8800 system in development for clinical phase programs. Matthew Myers, Catherine Johnsen, Jessica Taylor The analytical development group at Teva supports sample testing in formulation and process development and develops methods to transfer to quality control (QC) for use in clinical and commercial release labs. A system suitability assessment of the BioPhase 8800 system for Analytical Development During this phase of development, thousands of samples need to be analyzed by capillary electrophoresis (CE). In 2023, for example, the team tested over 4000 samples using CE on the PA 800 Plus system. Even though the team Analytical Development sits in development providing more freedom to operate utilizing new technologies, they must consider the transferability of methods to teams that are in QC and GMP labs. Demonstrating data equivalence between requires systems reduces the need to perform bridging studies. Pushing more of the middle work: The BioPhase 8800 system features 8 capillaries compared to the singlecapillary PA 800 Plus system. Establishing a strategy for how to treat capillaries is crucial for data reporting and system suitability. Teva decided to develop a system suitability for each individual capillary, treating each capillary as its own system. This approach offers several advantages: 1) Allows for each capillary to have its own set of controls 2) Allows one capillary to fail, and not affect the entire data set 3) Accounts for slight differences between capillaries 4) Accounts for minor errors in injections Specific to this evaluation, Capillary H consistently showed slightly higher peak area values across all injections compared to capillaries A to G (Figure 2). The use of one set of system suit Figure 1 Over 1 year of data results for control standards run on BioPhase 8800 system and PA 00 Plus system demonstrate an acceptable trend with less than 1% spread Figure 3 Overall run time of 8 samples displayed in minutes between the PA 800 Plus system and the BioPhase 8800 system across all 8 capillaries would have increased the risk of invalid results for all capillaries due to this systematic difference. With the capillaries being treated as separate systems with their own set of controls, differences in raw data can be accommodated and processed individually, relative to each capillaries associated control. Enhancing throughput: Although not fully exploiting the throughput of the BioPhase 8800 system, by treating each capillary individually this effectively provided the team with one single instrument that had the capacity of eight PA 800 Plus systems running in parallel and significantly increased data acquisition and sample throughput. The biggest gain the team experienced was overnight performance, while no one was in the lab. With the current SOP for the PA 800 Plus system, 8 samples take over 20 hours to run, whereas on the BioPhase 8800 system, 8 samples can be run in less than 7 hours. (figure 3)