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Re-examination of MAGE-A3 as a T-cell Therapeutic Target

J Immunother. 2021-04; 
Aaron D Martin, Xueyin Wang, Mark L Sandberg, Kathleen R Negri, Ming L Wu, Dora Toledo Warshaviak, Grant B Gabrelow, Michele E McElvain, Bella Lee, Mark E Daris, Han Xu, Alexander Kamb
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Peptide Synthesis … This subset encompasses ∼25,000 deaths/yr from cancer in the US … All peptides were purchased from GenScript by custom order … Serially diluted peptide solutions were added to T2 cells resuspended in peptide-loading media (Roswell Park Memorial Institute (RPMI) 1640 … Get A Quote

摘要

In 2013, an innovative MAGE-A3-directed cancer therapeutic of great potential value was terminated in the clinic because of neurotoxicity. The safety problems were hypothesized to originate from off-target T-cell receptor activity against a closely related MAGE-A12 peptide. A combination of published and new data led us to test this hypothesis with current technology. Our results call into question MAGE-A12 as the source of the neurotoxicity. Rather, the data imply that an alternative related peptide from EPS8L2 may be responsible. Given the qualities of MAGE-A3 as an onco-testis antigen widely expressed in tumors and largely absent from normal adult tissues, these findings suggest that MAGE-A3 may deserve furt... More

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