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Transient cell-in-cell formation underlies tumor resistance to immunotherapy
[article]
2020
bioRxiv
pre-print
Despite the remarkable success of immunotherapy in cancer, most patients will develop resistant tumors. While the main conceptual paradigm suggests that relapsed clones emerge through a process of clonal selection and immunoediting, currently little evidence directly demonstrates this process in epithelial cancers. To study this process, we established several mouse models in which tumors drastically regress following immunotherapy, yet resistant tumors relapse within a few weeks of treatment
doi:10.1101/2020.09.10.287441
fatcat:skfo7my7tvh6re5yldjrxhxorq