A lymphodepleted non-human primate model for the assessment of acute on-target and off-tumor toxicity of human chimeric antigen receptor-T cells
| Autor: | Hidemi Mochizuki, Miyuki Tanaka, Shigeki Yagyu, Kumiko Yamashima, Shoji Saito, Hiroshi Kubo, Akihito Shimoi, Kengo Sakamoto, Yozo Nakazawa |
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| Rok vydání: | 2020 |
| Předmět: |
0301 basic medicine
Cyclophosphamide medicine.medical_treatment Immunology Pharmacology Cell therapy 03 medical and health sciences 0302 clinical medicine In vivo medicine Immunology and Allergy CAR‐T cells Receptor on‐target toxicity General Nursing non‐human primate Chemotherapy business.industry lymphodepletion RC581-607 off‐target toxicity Chimeric antigen receptor Fludarabine 030104 developmental biology 030220 oncology & carcinogenesis Toxicity Original Article Immunologic diseases. Allergy cell therapy business medicine.drug |
| Zdroj: | Clinical & Translational Immunology Clinical & Translational Immunology, Vol 10, Iss 6, Pp n/a-n/a (2021) |
| ISSN: | 2050-0068 |
| Popis: | Objectives Chimeric antigen receptor (CAR)‐T cell therapy possesses the potential to cause unexpected on‐target toxicities that may be life‐threatening. Non‐human primates (NHPs) share considerable structural homology and expression profiles of most proteins with humans and are therefore utilised as an animal model for non‐clinical safety studies. We have developed a lymphodepleted NHP model by conditioning the animals with immunosuppressive chemotherapy designed to simulate clinical practice conditions, to induce transient mixed chimerism before the administration of human CAR‐T cells redirected to target Ephrin type‐B receptor 4 (EPHB4‐CAR‐T cells) to evaluate the toxicity of these cells. Methods We administered 60 mg m−2 day−1 of fludarabine for 4 days and 30 mg kg−1 day−1 of cyclophosphamide for 2 days intravenously to cynomolgus macaques for lymphodepletion; then, 3.3 × 106 kg−1 of non‐transduced or EPHB4‐CAR‐T cells was infused into the macaques, respectively. All macaques were closely monitored and evaluated for potential toxicity for 7 days. Results Lymphodepletion was successfully achieved on day −1 before T‐cell infusion and persisted over 7 days without severe organ toxicities. A single administration of human EPHB4‐CAR‐T cells did not induce overt organ toxicities, although EPHB4‐CAR‐T cells were activated in vivo as evidenced by the elevation in copy numbers of the CAR transgene 24 h after infusion. Conclusion Although this NHP model is limited for the full evaluation of toxicity of human CAR‐T cells and the conditioning protocol should be further optimised, this lymphodepleted NHP model could be used to assess acute on‐target/off‐tumor toxicities of CAR‐T cells. We have investigated the on‐target/off‐target toxicity of CAR‐T cells using a lymphodepleted non‐human primate (NHP) model. We followed the most widely accepted non‐myeloablative lymphodepletion protocol in clinical use for CAR‐T therapy to deplete the lymphocyte counts in the macaques, and lymphodepletion allowed CAR‐T cells to transiently expand and become detectable in the peripheral blood. Our lymphodepleted NHP model could provide new insights into the safety assessment of immune effector cell‐based therapy as the investigational new intervention. |
| Databáze: | OpenAIRE |
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