Yarmarkovich, Mark and Marshall, Quinlen F. and Warrington, John M. and Premaratne, Rasika and Farrel, Alvin and Groff, David and Li, Wei and di Marco, Moreno and Runbeck, Erin and Truong, Hau and Toor, Jugmohit S. and Tripathi, Sarvind and Nguyen, Son and Shen, Helena and Noel, Tiffany and Church, Nicole L. and Weiner, Amber and Kendsersky, Nathan and Martinez, Dan and Weisberg, Rebecca and Christie, Molly and Eisenlohr, Laurence and Bosse, Kristopher R. and Dimitrov, Dimiter S. and Stevanovic, Stefan and Sgourakis, Nikolaos G. and Kiefel, Ben R. and Maris, John M. (2023) Targeting of intracellular oncoproteins with peptide-centric CARs. Nature. ISSN 0028-0836
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Abstract
The majority of oncogenic drivers are intracellular proteins, constraining their immunotherapeutic targeting to mutated peptides (neoantigens) presented by individual human leukocyte antigen (HLA) allotypes1. However, most cancers have a modest mutational burden that is insufficient for generating responses using neoantigen-based therapies2,3. Neuroblastoma is a paediatric cancer that harbours few mutations and is instead driven by epigenetically deregulated transcriptional networks4. Here we show that the neuroblastoma immunopeptidome is enriched with peptides derived from proteins essential for tumorigenesis. We focused on targeting the unmutated peptide QYNPIRTTF discovered on HLA-A*24:02, which is derived from the neuroblastoma-dependency gene and master transcriptional regulator PHOX2B. To target QYNPIRTTF, we developed peptide-centric chimeric antigen receptors (PC-CARs) through a counter panning strategy using predicted potentially cross-reactive peptides. We further proposed that PC-CARs can recognize peptides on additional HLA allotypes when presenting a similar overall molecular surface. Informed by our computational modelling results, we show that PHOX2B PC-CARs also recognize QYNPIRTTF presented by HLA-A*23:01, the most common non-A2 allele in people with African ancestry. Finally, we demonstrate potent and specific killing of neuroblastoma cells expressing these HLAs in vitro and complete tumour regression in mice. These data suggest that PC-CARs have the potential to expand the pool of immunotherapeutic targets to include non-immunogenic intracellular oncoproteins and allow targeting through additional HLA allotypes in a clinical setting.
Item Type: | Article |
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Subjects: | European Repository > Multidisciplinary |
Depositing User: | Managing Editor |
Date Deposited: | 10 Nov 2023 04:12 |
Last Modified: | 10 Nov 2023 04:12 |
URI: | http://go7publish.com/id/eprint/3621 |