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B Cells and T Follicular Helper Cells Mediate Response to Checkpoint Inhibitors in High Mutation Burden Mouse Models of Breast Cancer
Author(s) -
Daniel P. Hollern,
Nuo Xu,
Aatish Thennavan,
Cherise Ryan Glodowski,
Susana GarcíaRecio,
Kevin R. Mott,
Xiaping He,
Joseph P. Garay,
Kelly Carey-Ewend,
David Marron,
John Ford,
Siyao Liu,
Sarah C. Vick,
Miguel Martín,
Joel S. Parker,
Benjamin G. Vincent,
Jonathan S. Serody,
Charles M. Perou
Publication year - 2019
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2019.10.028
Subject(s) - biology , cancer research , mutation , breast cancer , follicular phase , cancer , immunology , genetics , microbiology and biotechnology , gene
This study identifies mechanisms mediating responses to immune checkpoint inhibitors using mouse models of triple-negative breast cancer. By creating new mammary tumor models, we find that tumor mutation burden and specific immune cells are associated with response. Further, we developed a rich resource of single-cell RNA-seq and bulk mRNA-seq data of immunotherapy-treated and non-treated tumors from sensitive and resistant murine models. Using this, we uncover that immune checkpoint therapy induces T follicular helper cell activation of B cells to facilitate the anti-tumor response in these models. We also show that B cell activation of T cells and the generation of antibody are key to immunotherapy response and propose a new biomarker for immune checkpoint therapy. In total, this work presents resources of new preclinical models of breast cancer with large mRNA-seq and single-cell RNA-seq datasets annotated for sensitivity to therapy and uncovers new components of response to immune checkpoint inhibitors.

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