4.7 Article

Limited efficacy of APRIL CAR in patients with multiple myeloma indicate challenges in the use of natural ligands for CAR T-cell therapy

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BMJ PUBLISHING GROUP
DOI: 10.1136/jitc-2023-006699

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clinical trials as topic; immunotherapy; adoptive; T-lymphocytes

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In this study, a ligand-based CAR targeting two myeloma antigens was constructed and evaluated in a clinical trial. The results showed that the APRIL CAR was well tolerated, but the clinical responses were disappointing. Comparing with other BCMA CARs, the APRIL CAR exhibited functional deficiencies due to reduced target binding by cell-expressed ligand.
BackgroundWe used a proliferating ligand (APRIL) to construct a ligand-based third generation chimeric antigen receptor (CAR) able to target two myeloma antigens, B-cell maturation antigen (BCMA) and transmembrane activator and CAML interactor. MethodsThe APRIL CAR was evaluated in a Phase 1 clinical trial (NCT03287804, AUTO2) in patients with relapsed, refractory multiple myeloma. Eleven patients received 13 doses, the first 15x10(6) CARs, and subsequent patients received 75,225,600 and 900x10(6) CARs in a 3+3 escalation design. ResultsThe APRIL CAR was well tolerated. Five (45.5%) patients developed Grade 1 cytokine release syndrome and there was no neurotoxicity. However, responses were only observed in 45.5% patients (1xvery good partial response, 3xpartial response, 1xminimal response). Exploring the mechanistic basis for poor responses, we then compared the APRIL CAR to two other BCMA CARs in a series of in vitro assays, observing reduced interleukin-2 secretion and lack of sustained tumor control by APRIL CAR regardless of transduction method or co-stimulatory domain. There was also impaired interferon signaling of APRIL CAR and no evidence of autoactivation. Thus focusing on APRIL itself, we confirmed similar affinity to BCMA and protein stability in comparison to BCMA CAR binders but reduced binding by cell-expressed APRIL to soluble BCMA and reduced avidity to tumor cells. This indicated either suboptimal folding or stability of membrane-bound APRIL attenuating CAR activation. ConclusionsThe APRIL CAR was well tolerated, but the clinical responses observed in AUTO2 were disappointing. Subsequently, when comparing the APRIL CAR to other BCMA CARs, we observed in vitro functional deficiencies due to reduced target binding by cell-expressed ligand.

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