LILRB1-HLA-G Axis Defines a Checkpoint Driving Natural Killer Cell Exhaustion in Tuberculosis

Overview

Journal EMBO Mol Med

Specialty Molecular Biology

Date 2024 Jul 19

PMID 39030302

Authors

Jing Wang

Qiyao Chai

Zehui Lei

Yiru Wang

Jiehua He

Pupu Ge

Zhe Lu

Lihua Qiang

Dongdong Zhao

Shanshan Yu

Changgen Qiu

Yanzhao Zhong

Bing-Xi Li

Lingqiang Zhang

Yu Pang

George Fu Gao

Cui Hua Liu

Affiliations

Soon will be listed here.

Abstract

Chronic infections, including Mycobacterium tuberculosis (Mtb)-caused tuberculosis (TB), can induce host immune exhaustion. However, the key checkpoint molecules involved in this process and the underlying regulatory mechanisms remain largely undefined, which impede the application of checkpoint-based immunotherapy in infectious diseases. Here, through adopting time-of-flight mass cytometry and transcriptional profiling to systematically analyze natural killer (NK) cell surface receptors, we identify leukocyte immunoglobulin like receptor B1 (LILRB1) as a critical checkpoint receptor that defines a TB-associated cell subset (LILRB1 NK cells) and drives NK cell exhaustion in TB. Mechanistically, Mtb-infected macrophages display high expression of human leukocyte antigen-G (HLA-G), which upregulates and activates LILRB1 on NK cells to impair their functions by inhibiting mitogen-activated protein kinase (MAPK) signaling via tyrosine phosphatases SHP1/2. Furthermore, LILRB1 blockade restores NK cell-dependent anti-Mtb immunity in immuno-humanized mice. Thus, LILRB1-HLA-G axis constitutes a NK cell immune checkpoint in TB and serves as a promising immunotherapy target.

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