A closed, autologous bioprocess optimized for TCR‐T cell therapies

生物过程 细胞疗法 生物过程工程 生物反应器 细胞生长 细胞 T细胞 生物 记忆T细胞 细胞生物学 化学 免疫学 免疫系统 生物技术 生物化学 古生物学 植物
作者
Yijun Liu,Eugenia Zah,Carlos Arbelaez,Hae Jin Kim,Edwige Gros,Ranelle Buck,Kayley Cox,Sungeun Kim,Martina Kopp,Kathryn Henckels,Jennitte Stevens
出处
期刊:Biotechnology and Bioengineering [Wiley]
卷期号:120 (7): 1809-1821 被引量:2
标识
DOI:10.1002/bit.28389
摘要

Abstract Autologous cell therapy has proven to be an effective treatment for hematological malignancies. Cell therapies for solid tumors are on the horizon, however the high cost and complexity of manufacturing these therapies remain a challenge. Routinely used open steps to transfer cells and reagents through unit operations further burden the workflow reducing efficiency and increasing the chance for human error. Here we describe a fully closed, autologous bioprocess generating engineered TCR‐T cells. This bioprocess yielded 5–12 × 10e9 TCR‐expressing T cells, transduced at low multiplicity of infections, within 7–10 days, and cells exhibited an enriched memory T‐cell phenotype and enhanced metabolic fitness. It was demonstrated that activating, transducing, and expanding leukapheresed cells in a bioreactor without any T‐cell or peripheral blood mononuclear cell enrichment steps had a high level of T‐cell purity (~97%). Several critical process parameters of the bioreactor, including culturing at a high cell density (7e6 cells/mL), adjusting rocking agitations during phases of scale‐up, lowering glycolysis through the addition of 2‐deoxy‐ d ‐glucose, and modulating interleukin‐2 levels, were investigated on their roles in regulating transduction efficiency, cell growth, and T‐cell fitness such as T‐cell memory phenotype and resistance to activation‐induced cell death. The bioprocess described herein supports scale‐out feasibility by enabling the processing of multiple patients' batches in parallel within a Grade C cleanroom.
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