Blockade of Immune-Checkpoint B7-H4 and Lysine Demethylase 5B in Esophageal Squamous Cell Carcinoma Confers Protective Immunity Against Infection

Overview

Journal Cancer Immunol Res

Specialties Allergy & Immunology
Oncology

Date 2019 Jul 28

PMID 31350278

Citations 20

Authors

Xiang Yuan

Yiwen Liu

Guifang Li

Zijun Lan

Mingyang Ma

Huaxu Li

Jinyu Kong

Jiangtao Sun

Gaochao Hou

Xurong Hou

Yingjian Ma

Feng Ren

Fuyou Zhou

Shegan Gao

Affiliations

Soon will be listed here.

Abstract

Pathogens are capable of hijacking immune defense mechanisms, thereby creating a tolerogenic environment for hypermutated malignant cells that arise within the site of infection. Immune checkpoint-oriented immunotherapies have shown considerable promise. Equally important, the epigenetic reprogramming of an immune-evasive phenotype that activates the immune system in a synergistic manner can improve immunotherapy outcomes. These advances have led to combinations of epigenetic- and immune-based therapeutics. We previously demonstrated that isolated from esophageal squamous cell carcinoma (ESCC) lesions represents a major pathogen associated with this deadly disease. In this study, we examined the mechanisms associated with host immunity during infection and demonstrated that experimentally infected ESCC responds by increasing the expression of B7-H4 and lysine demethylase 5B, which allowed subsequent analysis of the immunotherapeutic effects of anti-B7-H4 and histone demethylase inhibitors in models of chronic infection and immunity against xenografted human tumors. Using three different preclinical mouse models receiving combined therapy, we showed that mice mounted strong resistance against infection and tumor challenge. This may have occurred via generation of a T cell-mediated response in the microenvironment and formation of immune memory. In ESCC subjects, coexpression of B7-H4 and KDM5B correlated more significantly with bacterial load than with the expression of either molecule alone. These results highlight the unique ability of to evade immunity and define potential targets that can be exploited therapeutically to improve the control of infection and the development of associated neoplasia.

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