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Development of a cGMP-compliant process to manufacture donor-derived, CD45RA-depleted memory CD19-CAR T cells

by Velasquez, M. Paulina , Zhou, Sheng , Lockey, Timothy , Moore, Jennifer , Métais, Jean-Yves , Gottschalk, Stephen , Zheng, Fei , Meagher, Michael M , Park, Jeoungeun J , Akel, Salem , Willis, Catherine , Shang, Na , Triplett, Brandon M , Kim-Hoehamer, Young-In , Riberdy, Janice M , Talleur, Aimee C

in Antigens / Antitumor activity / CD19 antigen / CD4 antigen / CD45RA antigen / Cell culture / Cell therapy / Chimeric antigen receptors / Cryopreservation / Good Manufacturing Practice / Immunological memory / Lymphocytes / Lymphocytes B / Lymphocytes T / Malignancy / Manufacturing / Memory cells / Phenotypes / Tissue engineering

2023

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Development of a cGMP-compliant process to manufacture donor-derived, CD45RA-depleted memory CD19-CAR T cells

2023

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Development of a cGMP-compliant process to manufacture donor-derived, CD45RA-depleted memory CD19-CAR T cells

2023

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Journal Article

Development of a cGMP-compliant process to manufacture donor-derived, CD45RA-depleted memory CD19-CAR T cells

Velasquez, M. Paulina,

Zhou, Sheng,

Lockey, Timothy,

Moore, Jennifer,

Métais, Jean-Yves,

Gottschalk, Stephen,

Zheng, Fei,

Meagher, Michael M,

Park, Jeoungeun J,

Akel, Salem,

Willis, Catherine,

Shang, Na,

Triplett, Brandon M,

Kim-Hoehamer, Young-In,

Riberdy, Janice M,

Talleur, Aimee C

2023

Overview

Autologous chimeric antigen receptor (CAR) T cells targeting the CD19 antigen have demonstrated a high complete response rate in relapsed/refractory B-cell malignancies. However, autologous CAR T cell therapy is not an option for all patients. Here we optimized conditions for clinical-grade manufacturing of allogeneic CD19-CAR T cells using CD45RA-depleted donor memory T cells (Tm) for a planned clinical trial. Tm were activated using the MACS GMP T Cell TransAct reagent and transduced in the presence of LentiBOOST with a clinical-grade lentiviral vector that encodes a 2nd generation CD19-CAR with a 41BB.zeta endodomain. Transduced T cells were transferred to a G-Rex cell culture device for expansion and harvested on day 7 or 8 for cryopreservation. The resulting CD19-CAR(Mem) T cells expanded on average 34.2-fold, and mean CAR expression was 45.5%. The majority of T cells were CD4+ and had a central memory or effector memory phenotype, and retained viral specificity. CD19-CAR(Mem) T cells recognized and killed CD19-positive target cells in vitro and had potent antitumor activity in an ALL xenograft model. Thus we have successfully developed a current good manufacturing practice-compliant process to manufacture donor-derived CD19-CAR(Mem) T cells. Our manufacturing process could be readily adapted for CAR(Mem) T cells targeting other antigens.

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Nature Publishing Group

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