Article Synopsis
- Genetically modified T cells, known as CAR T cells, show strong responses against certain targets in blood cancers, but their effectiveness in solid tumors is limited due to a lack of specific antigens.
- Researchers identified that abnormal self-antigens, like the Tn glycoform of MUC1, can be effective targets for cancer treatment.
- Anti-Tn-MUC1 CAR T cells effectively killed cancer cells and controlled tumor growth in models of T cell leukemia and pancreatic cancer, highlighting the potential of targeting unique antigens for therapy.
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Article Abstract
Genetically modified T cells expressing chimeric antigen receptors (CARs) demonstrate robust responses against lineage restricted, non-essential targets in hematologic cancers. However, in solid tumors, the full potential of CAR T cell therapy is limited by the availability of cell surface antigens with sufficient cancer-specific expression. The majority of CAR targets have been normal self-antigens on dispensable hematopoietic tissues or overexpressed shared antigens. Here, we established that abnormal self-antigens can serve as targets for tumor rejection. We developed a CAR that recognized cancer-associated Tn glycoform of MUC1, a neoantigen expressed in a variety of cancers. Anti-Tn-MUC1 CAR T cells demonstrated target-specific cytotoxicity and successfully controlled tumor growth in xenograft models of T cell leukemia and pancreatic cancer. These findings demonstrate the therapeutic efficacy of CAR T cells directed against Tn-MUC1 and present aberrantly glycosylated antigens as a novel class of targets for tumor therapy with engineered T cells.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5358667 | PMC |
| http://dx.doi.org/10.1016/j.immuni.2016.05.014 | DOI Listing |