1. Choice of activation protocol impacts the yield and quality of CAR T cell product, particularly with older individuals.
- Author
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Mehta, Palak H, Trollope, Gemma S, Leung, Patrick, Chinni, Shivali Savita, Iasinskaia, Anna, Harrison, Aaron J, Hughes‐Parry, Hannah, Jenkins, Misty R, Kershaw, Michael H, Jaworowski, Anthony, Slaney, Clare Y, Koldej, Rachel M, Ritchie, David S, and Quinn, Kylie M
- Subjects
MONONUCLEAR leukocytes ,T cell differentiation ,T cells ,OLDER people ,CHIMERIC antigen receptors - Abstract
Objectives: In clinical chimeric antigen receptor (CAR) T cell therapy, one of the strongest correlates of favorable patient responses is lower levels of differentiation in T cells from the peripheral blood mononuclear cell (PBMC) starting material or the CAR T cell product. T cells from older patients are inherently more differentiated, but we hypothesised that specific activation protocols could be used to limit CAR T cell differentiation during manufacturing, particularly in older patients. Methods: We used PBMCs from young (20–30 years old) and older (60+ years old) healthy donors to generate CAR T cells using two activation protocols: soluble anti‐(α) CD3 monoclonal antibody (mAb) vs immune complexes of αCD3 and αCD28 mAbs. Products were assessed for yield, function and differentiation, which was used as a measure of CAR T cell quality. T cells in PBMCs were assessed for CD28 expression and correlative analyses were performed. Results: Older samples generated fewer, more differentiated CAR T cells than young samples, and the αCD3/CD28 mAb protocol exacerbated this, further reducing yield and quality. CD28 expression by T cells correlated with CAR T cell differentiation, but T cell differentiation in PBMC starting material was a stronger correlate of CAR T cell differentiation. Conclusions: Choice of activation protocol can substantially impact on the yield and quality of CAR T cells during manufacturing. This is a key consideration for older patients whose samples already generate a poorer yield and lower quality of CAR T cells. [ABSTRACT FROM AUTHOR]
- Published
- 2024
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