LILRB4 suppresses immunity in solid tumors and is a potential target for immunotherapy

Author:

Sharma Naveen1ORCID,Atolagbe Oluwatomisin T.1ORCID,Ge Zhongqi1ORCID,Allison James P.123ORCID

Affiliation:

1. Department of Immunology, The University of Texas MD Anderson Cancer Center, Houston, TX

2. Immunotherapy Platform, The University of Texas MD Anderson Cancer Center, Houston, TX

3. Parker Institute for Cancer Immunotherapy, The University of Texas MD Anderson Cancer Center, Houston, TX

Abstract

Immune receptors expressed on TAMs are intriguing targets for tumor immunotherapy. In this study, we found inhibitory receptor LILRB4 on a variety of intratumoral immune cell types in murine tumor models and human cancers, most prominently on TAMs. LILRB4, known as gp49B in mice, is a LILRB family receptor. Human and murine LILRB4 have two extracellular domains but differ in the number of intracellular ITIMs (three versus two). We observed a high correlation in LILRB4 expression with other immune inhibitory receptors. After tumor challenge, LILRB4−/− mice and mice treated with anti-LILRB4 antibody showed reduced tumor burden and increased survival. LILRB4−/− genotype or LILRB4 blockade increased tumor immune infiltrates and the effector (Teff) to regulatory (Treg) T cell ratio and modulated phenotypes of TAMs toward less suppressive, CD4+ T cells to Th1 effector, and CD8+ T cells to less exhausted. These findings reveal that LILRB4 strongly suppresses tumor immunity in TME and that alleviating that suppression provides antitumor efficacy.

Funder

Cancer Prevention and Research Institute of Texas

Publisher

Rockefeller University Press

Subject

Immunology,Immunology and Allergy

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