| Literature DB >> 35803260 |
Adrienne M Luoma1, Shengbao Suo2, Yifan Wang3, Lauren Gunasti4, Caroline B M Porter5, Nancy Nabilsi3, Jenny Tadros3, Andrew P Ferretti3, Sida Liao3, Cagan Gurer3, Yu-Hui Chen6, Shana Criscitiello4, Cora A Ricker7, Danielle Dionne5, Orit Rozenblatt-Rosen5, Ravindra Uppaluri8, Robert I Haddad7, Orr Ashenberg5, Aviv Regev9, Eliezer M Van Allen7, Gavin MacBeath3, Jonathan D Schoenfeld10, Kai W Wucherpfennig11.
Abstract
Neoadjuvant immune checkpoint blockade has shown promising clinical activity. Here, we characterized early kinetics in tumor-infiltrating and circulating immune cells in oral cancer patients treated with neoadjuvant anti-PD-1 or anti-PD-1/CTLA-4 in a clinical trial (NCT02919683). Tumor-infiltrating CD8 T cells that clonally expanded during immunotherapy expressed elevated tissue-resident memory and cytotoxicity programs, which were already active prior to therapy, supporting the capacity for rapid response. Systematic target discovery revealed that treatment-expanded tumor T cell clones in responding patients recognized several self-antigens, including the cancer-specific antigen MAGEA1. Treatment also induced a systemic immune response characterized by expansion of activated T cells enriched for tumor-infiltrating T cell clonotypes, including both pre-existing and emergent clonotypes undetectable prior to therapy. The frequency of activated blood CD8 T cells, notably pre-treatment PD-1-positive KLRG1-negative T cells, was strongly associated with intra-tumoral pathological response. These results demonstrate how neoadjuvant checkpoint blockade induces local and systemic tumor immunity.Entities:
Keywords: T cells; cancer; immunotherapy; neoadjuvant therapy; single-cell RNA sequencing; tissue-resident memory T cells
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Year: 2022 PMID: 35803260 PMCID: PMC9508682 DOI: 10.1016/j.cell.2022.06.018
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 66.850