Cell Reports (Oct 2021)

Targeting TREM2 on tumor-associated macrophages enhances immunotherapy

  • Mikhail Binnewies,
  • Joshua L. Pollack,
  • Joshua Rudolph,
  • Subhadra Dash,
  • Marwan Abushawish,
  • Tian Lee,
  • Nadine S. Jahchan,
  • Pamela Canaday,
  • Erick Lu,
  • Manith Norng,
  • Shilpa Mankikar,
  • Victoria M. Liu,
  • Xiaoyan Du,
  • Amanda Chen,
  • Ranna Mehta,
  • Rachael Palmer,
  • Vladislava Juric,
  • Linda Liang,
  • Kevin P. Baker,
  • Leonard Reyno,
  • Matthew F. Krummel,
  • Michel Streuli,
  • Venkataraman Sriram

Journal volume & issue
Vol. 37, no. 3
p. 109844

Abstract

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Summary: Converting checkpoint inhibitor (CPI)-resistant individuals to being responsive requires identifying suppressive mechanisms. We identify TREM2+ tumor-associated macrophages (TAMs) as being correlated with exhausted CD8+ tumor-infiltrating lymphocytes (TILs) in mouse syngeneic tumor models and human solid tumors of multiple histological types. Fc domain-enhanced anti-TREM2 monoclonal antibody (mAb) therapy promotes anti-tumor immunity by elimination and modulation of TAM populations, which leads to enhanced CD8+ TIL infiltration and effector function. TREM2+ TAMs are most enriched in individuals with ovarian cancer, where TREM2 expression corresponds to disease grade accompanied by worse recurrence-free survival. In an aggressive orthotopic ovarian cancer model, anti-TREM2 mAb therapy drives potent anti-tumor immunity. These results highlight TREM2 as a highly attractive target for immunotherapy modulation in individuals who are refractory to CPI therapy and likely have a TAM-rich tumor microenvironment.

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