| Literature DB >> 35447074 |
Pilar Baldominos1, Alex Barbera-Mourelle2, Olga Barreiro3, Yu Huang4, Andrew Wight4, Jae-Won Cho5, Xi Zhao1, Guillem Estivill1, Isam Adam1, Xavier Sanchez4, Shannon McCarthy6, Julien Schaller1, Zara Khan1, Albert Ruzo1, Ricardo Pastorello7, Edward T Richardson8, Deborah Dillon9, Paula Montero-Llopis10, Romualdo Barroso-Sousa11, Juliet Forman12, Sachet A Shukla13, Sara M Tolaney14, Elizabeth A Mittendorf7, Ulrich H von Andrian15, Kai W Wucherpfennig16, Martin Hemberg5, Judith Agudo17.
Abstract
Immunotherapy is a promising treatment for triple-negative breast cancer (TNBC), but patients relapse, highlighting the need to understand the mechanisms of resistance. We discovered that in primary breast cancer, tumor cells that resist T cell attack are quiescent. Quiescent cancer cells (QCCs) form clusters with reduced immune infiltration. They also display superior tumorigenic capacity and higher expression of chemotherapy resistance and stemness genes. We adapted single-cell RNA-sequencing with precise spatial resolution to profile infiltrating cells inside and outside the QCC niche. This transcriptomic analysis revealed hypoxia-induced programs and identified more exhausted T cells, tumor-protective fibroblasts, and dysfunctional dendritic cells inside clusters of QCCs. This uncovered differential phenotypes in infiltrating cells based on their intra-tumor location. Thus, QCCs constitute immunotherapy-resistant reservoirs by orchestrating a local hypoxic immune-suppressive milieu that blocks T cell function. Eliminating QCCs holds the promise to counteract immunotherapy resistance and prevent disease recurrence in TNBC.Entities:
Keywords: T cells; TME; breast cancer; cancer-associated fibroblasts; dendritic cells; immunotherapy; resistance to therapy; single-cell RNA-sequencing; tumor dormancy; tumor immunology; tumor microenvironment
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Year: 2022 PMID: 35447074 DOI: 10.1016/j.cell.2022.03.033
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 66.850