Tumor Endothelial Cell-induced CD8 T-cell Exhaustion Via GPNMB in Hepatocellular Carcinoma

Overview

Journal Cancer Sci

Specialty Oncology

Date 2022 Mar 15

PMID 35289033

Authors

Yoshihiro Sakano

Takehiro Noda

Shogo Kobayashi

Kazuki Sasaki

Yoshifumi Iwagami

Daisaku Yamada

Yoshito Tomimaru

Hirofumi Akita

Kunihito Gotoh

Hidenori Takahashi

Tadafumi Asaoka

Masahiro Tanemura

Hisashi Wada

Yuichiro Doki

Hidetoshi Eguchi

Affiliations

Soon will be listed here.

Abstract

Tumor endothelial cells (TECs) promote tumor angiogenesis and regulate cytotoxic T cells in the tumor microenvironment. However, the roles of TECs for tumor-infiltrating T-cell in hepatocellular carcinoma (HCC) is still unknown. Here, we aimed to investigate how TECs influenced tumor growth and immune responses of HCC focusing on CD8 T-cell infiltration and exhaustion. First, TECs were isolated from subcutaneous HCC tumors with murine HCC cell lines (BNL-T) with magnetic selection of CD31 cells, and normal endothelial cells (NECs) were isolated from normal liver. Second, immunocompetent mice were injected with BNL-T alone, BNL-T + NECs, or BNL-T + TECs for tumor formation, and the functions and exhaustion of tumor-infiltrating CD8 T cells were evaluated. The mice injected with BNL-T + TEC showed rapid tumorigenesis and a decrease in the number of infiltrating CD8 T cells. In addition, the percentage of CD8 T-cell exhaustion was significantly higher in tumors from the administration of BNL-T + TEC. Third, the next-generation sequencing on TECs was performed to identify mRNAs that might be a novel treatment target. The molecule of glycoprotein nonmetastatic melanoma protein B (GPNMB) was identified and the functions of GPNMB was analyzed by silencing of GPNMB expression using small interfering RNAs. The silencing of GPNMB expression in TECs induced the suppression of tumor growth and T-cell exhaustion. In conclusion, TECs induced tumor-infiltrating T-cell exhaustion via GPNMB expression and GPNMB might be a novel therapeutic target in HCC.

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