Cancer Regression and Neurological Toxicity Following Anti-MAGE-A3 TCR Gene Therapy

Abstract: Nine cancer patients were treated with adoptive cell therapy using autologous anti-MAGE-A3 TCR engineered T cells. Five patients experienced clinical regression of their cancers including two on-going responders. Beginning 1–2 days post-infusion, three patients (#’s 5, 7, and 8) experienced mental status changes, and two patients (5 and 8) lapsed into comas and subsequently died. Magnetic resonance imagining analysis of patients 5 and 8 demonstrated periventricular leukomalacia, and examination of their brains… Show more

“…Indeed, engineered T-cells demonstrated higher affinity for the HLA-A*0201-restricted epitope K MA ELVHFL of MAGE-A12 than for the targeted K VA ELVHFL epitope of MAGE-A3. 40 Peptide #31 (used to re-stimulate PBMCs in our ELISpot) contained the sequence K VA ELVHFL. In our study, four primates had specific immune responses to the fully conserved peptide 31.…”

“…Transfusion of engineered anti-MAGE-A3 CD8 + T-cells resulted in clinical regressions of tumors, but this treatment was deemed unsafe due to the aforementioned neurotoxocity. 40 Anti-MAGE-A3 vaccination has also been evaluated clinically using a recombinant protein strategy and, although this treatment was safe, no survival advantage was conferred. However, the induction of T-cell responses was not reported, precluding full assessment of this platform’s immunogenicity.…”

Preclinical evaluation of a MAGE-A3 vaccination utilizing the oncolytic Maraba virus currently in first-in-human trials

“…Indeed, engineered T-cells demonstrated higher affinity for the HLA-A*0201-restricted epitope K MA ELVHFL of MAGE-A12 than for the targeted K VA ELVHFL epitope of MAGE-A3. 40 Peptide #31 (used to re-stimulate PBMCs in our ELISpot) contained the sequence K VA ELVHFL. In our study, four primates had specific immune responses to the fully conserved peptide 31.…”

“…Transfusion of engineered anti-MAGE-A3 CD8 + T-cells resulted in clinical regressions of tumors, but this treatment was deemed unsafe due to the aforementioned neurotoxocity. 40 Anti-MAGE-A3 vaccination has also been evaluated clinically using a recombinant protein strategy and, although this treatment was safe, no survival advantage was conferred. However, the induction of T-cell responses was not reported, precluding full assessment of this platform’s immunogenicity.…”

Preclinical evaluation of a MAGE-A3 vaccination utilizing the oncolytic Maraba virus currently in first-in-human trials

“…Despite robust antitumor immunity using TCRs targeting diverse cancer antigens, there are severe unanticipated adverse effects resulting from T cell recognition of tissue-specific antigens gp100 and MART-1 expressed by both normal melanocytes and melanoma [203], or from the cross-reactivity of higher affinity MAGE-A3 TCR-transduced T cells against epitopes in unintended targets in normal and essential tissues [204,205]. Vaccination of cancer patients with gp100 and MART-1 resulted in objective clinical response without serious toxicity to melanocytes [182,185].…”

Immune targets and neoantigens for cancer immunotherapy and precision medicine

“…For instance, the neurological toxicity of anti-MAGE-A3 TCR gene therapy (also recognizing MAGE-A9 and A12 epitopes) might be related to unreported MAGE-A12 expression in brain. 22 The uncertainty over antigen expression patterns in normal tissue implies a need for systematic monitoring of potential toxicity.…”

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