Glioblastoma-Infiltrating CD8+ T Cells Are Predominantly a Clonally Expanded GZMK+ Effector Population.

Albert H Kim,Alexandra J Livingstone,Allegra A Petti,Anthony Z Wang,Bob S Carter,Bryan D Choi,Bryce L Mashimo,Daniel P Cahill,Eric C Leuthardt,Gavin P Dunn,Joseph D Bradley,Joshua L Dowling,Lydia A Leavitt,Mao Li,Markus I Anzaldua-Campos,Maximilian O Schaettler,Michael R Chicoine,Ngima D Sherpa,Pamela S Jones,Saad M Khan,Tanner M Johanns

doi:10.1158/2159-8290.cd-23-0913

Glioblastoma-Infiltrating CD8+ T Cells Are Predominantly a Clonally Expanded GZMK+ Effector Population.

Albert H Kim, Alexandra J Livingstone + Show 19 more

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https://doi.org/10.1158/2159-8290.cd-23-0913

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Journal: Cancer Discovery

Publication Date: Feb 27, 2024

Affiliation: University of Washington, University of Louisville, Harvard University

#Effector Population #Efficacy Of Blockade + Show 4 more

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Abstract

To understand the limited efficacy of immune-checkpoint blockade in GBM, we applied a multiomics approach to understand the TIL landscape. By highlighting the enrichment of GZMK+ effector T cells and the lack of exhausted T cells, we provide a new potential mechanism of resistance to immunotherapy in GBM. This article is featured in Selected Articles from This Issue, p. 897.

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