C3aR Signaling Inhibits NK-cell Infiltration into the Tumor Microenvironment in Mouse Models

肿瘤微环境 渗透(HVAC) 癌症研究 免疫疗法 生物 免疫系统 免疫学 细胞生物学 医学 物理 热力学
作者
Saravanan Nandagopal,Caiyun G. Li,Yü Xu,Quaovi H. Sodji,Edward E. Graves,Amato J. Giaccia
出处
期刊:Cancer immunology research [American Association for Cancer Research]
卷期号:10 (2): 245-258 被引量:20
标识
DOI:10.1158/2326-6066.cir-21-0435
摘要

Many solid tumors have low levels of cytotoxic CD56dim natural killer (NK) cells, suggesting that CD56dim NK-cell exclusion from the tumor microenvironment (TME) contributes to the decreased response rate of immunotherapy. Complement component 3a (C3a) is known for its tumor-promoting and immunosuppressive roles in solid tumors. Previous reports have implicated the involvement of the C3a receptor (C3aR) in immune cell trafficking into the TME. C3aR is predominantly expressed on the surface of activated cytotoxic NK cells, but a specific role for C3aR in NK-cell biology has not been investigated. Because solid tumors generate elevated C3a and have decreased NK-cell infiltration, we hypothesized that C3aR might play a role in cytotoxic NK-cell recruitment into the TME. Our results indicate that blocking C3aR signaling in NK cells increased NK-cell infiltration into the TME in mouse models and led to tumor regression. Because the critical lymphocyte trafficking integrin LFA-1 orchestrates the migration of activated NK cells, we wanted to gain insight into the interaction between C3aR signaling and LFA-1. Our results demonstrated that direct interaction between C3aR and LFA-1, which led to a high-affinity LFA-1 conformation, decreased NK-cell infiltration into the TME. We propose that approaches to enhance cytotoxic NK-cell infiltration into the TME, through either disrupting C3a and C3aR interaction or inhibiting the formation of high-affinity LFA-1, represent a new strategy to improve the efficiency of immunotherapy for cancer treatment.
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