| Literature DB >> 30778252 |
Brian C Miller1,2,3,4,5, Debattama R Sen1,3,6, Rose Al Abosy1,3, Kevin Bi1,3, Yamini V Virkud7, Martin W LaFleur1,3,4,5,6, Kathleen B Yates1,3, Ana Lako8, Kristen Felt8, Girish S Naik8, Michael Manos2,8, Evisa Gjini2,8, Juhi R Kuchroo4,5,6, Jeffrey J Ishizuka1,2,3, Jenna L Collier1,3,4,5,6, Gabriel K Griffin1,3,9, Seth Maleri4,5, Dawn E Comstock1,3,6, Sarah A Weiss1,3,6, Flavian D Brown1,3,4,5,6, Arpit Panda1,3, Margaret D Zimmer3, Robert T Manguso3, F Stephen Hodi2,8, Scott J Rodig8,9, Arlene H Sharpe3,4,5,6, W Nicholas Haining10,11,12.
Abstract
T cell dysfunction is a hallmark of many cancers, but the basis for T cell dysfunction and the mechanisms by which antibody blockade of the inhibitory receptor PD-1 (anti-PD-1) reinvigorates T cells are not fully understood. Here we show that such therapy acts on a specific subpopulation of exhausted CD8+ tumor-infiltrating lymphocytes (TILs). Dysfunctional CD8+ TILs possess canonical epigenetic and transcriptional features of exhaustion that mirror those seen in chronic viral infection. Exhausted CD8+ TILs include a subpopulation of 'progenitor exhausted' cells that retain polyfunctionality, persist long term and differentiate into 'terminally exhausted' TILs. Consequently, progenitor exhausted CD8+ TILs are better able to control tumor growth than are terminally exhausted T cells. Progenitor exhausted TILs can respond to anti-PD-1 therapy, but terminally exhausted TILs cannot. Patients with melanoma who have a higher percentage of progenitor exhausted cells experience a longer duration of response to checkpoint-blockade therapy. Thus, approaches to expand the population of progenitor exhausted CD8+ T cells might be an important component of improving the response to checkpoint blockade.Entities:
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Year: 2019 PMID: 30778252 PMCID: PMC6673650 DOI: 10.1038/s41590-019-0312-6
Source DB: PubMed Journal: Nat Immunol ISSN: 1529-2908 Impact factor: 25.606