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Antigen dominance hierarchies shape TCF1+ progenitor CD8 T cell phenotypes in tumors

Author(s)
Burger, Megan L; Cruz, Amanda M; Crossland, Grace E; Gaglia, Giorgio; Ritch, Cecily C; Blatt, Sarah E; Bhutkar, Arjun; Canner, David; Kienka, Tamina; Tavana, Sara Z; Barandiaran, Alexia L; Garmilla, Andrea; Schenkel, Jason M; Hillman, Michelle; de los Rios Kobara, Izumi; Li, Amy; Jaeger, Alex M; Hwang, William L; Westcott, Peter MK; Manos, Michael P; Holovatska, Marta M; Hodi, F Stephen; Regev, Aviv; Santagata, Sandro; Jacks, Tyler; ... Show more Show less
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Abstract
CD8 T cell responses against different tumor neoantigens occur simultaneously, yet little is known about the interplay between responses and its impact on T cell function and tumor control. In mouse lung adenocarcinoma, we found that immunodominance is established in tumors, wherein CD8 T cell expansion is predominantly driven by the antigen that most stably binds MHC. T cells responding to subdominant antigens were enriched for a TCF1+ progenitor phenotype correlated with response to immune checkpoint blockade (ICB) therapy. However, the subdominant T cell response did not preferentially benefit from ICB due to a dysfunctional subset of TCF1+ cells marked by CCR6 and Tc17 differentiation. Analysis of human samples and sequencing datasets revealed that CCR6+ TCF1+ cells exist across human cancers and are not correlated with ICB response. Vaccination eliminated CCR6+ TCF1+ cells and dramatically improved the subdominant response, highlighting a strategy to optimally engage concurrent neoantigen responses against tumors.
Date issued
2021
URI
https://hdl.handle.net/1721.1/146816
Department
Massachusetts Institute of Technology. Department of Biology
Journal
Cell
Publisher
Elsevier BV
Citation
Burger, Megan L, Cruz, Amanda M, Crossland, Grace E, Gaglia, Giorgio, Ritch, Cecily C et al. 2021. "Antigen dominance hierarchies shape TCF1+ progenitor CD8 T cell phenotypes in tumors." Cell, 184 (19).
Version: Author's final manuscript

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