Targeting LAIR1-mediated immunosuppression adds a new weapon to our immunotherapy arsenal
Ezri P. Perrin, Hannah K. Dorando, Jacqueline E. Payton
Ezri P. Perrin, Hannah K. Dorando, Jacqueline E. Payton
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Commentary

Targeting LAIR1-mediated immunosuppression adds a new weapon to our immunotherapy arsenal

Abstract

Leukocyte-associated Ig-like receptor 1 (LAIR1) is a collagen-binding inhibitory immune receptor that negatively regulates cellular activation. In this issue of the JCI, Tao et al. show that LAIR1-inhibitory signaling plays an important role in immunosuppressive M2-like tumor-associated macrophages (TAMs) in aggressive brain tumors. LAIR1 KO, antibody blockade, and an immunotherapy that incorporates a LAIR1-inhibitory module into a chimeric antigen receptor (CAR) all led to increased antitumor activity by CAR T cells, reduced M2-like TAMs, altered collagen networks, and increased survival rates in mouse tumor models. These findings demonstrate an innovative immunotherapeutic approach for cancer that leverages LAIR1 inhibition to combat multiple tumor immune evasion strategies.

Authors

Ezri P. Perrin, Hannah K. Dorando, Jacqueline E. Payton

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