CD106 in Tumor-Specific Exhausted CD8+ T Cells Mediates Immunosuppression by Inhibiting TCR Signaling

Yuto Naoi; Takao Morinaga; Joji Nagasaki; Ryo Ariyasu; Youki Ueda; Kazuo Yamashita; Wenhao Zhou; Shusuke Kawashima; Katsushige Kawase; Akiko Honobe‐Tabuchi; Takehiro Ohnuma; Tatsuyoshi Kawamura; Yoshiyasu Umeda; Yu Kawahara; Yasuhiro Nakamura; Yukiko Kiniwa; Osamu Yamasaki; Satoshi Fukushima; Masahito Kawazu; Yutaka Suzuki; Hiroyoshi Nishikawa; Toyoyuki Hanazawa; Mizuo Ando; Takashi Inozume; Yosuke Togashi

doi:10.1158/0008-5472.can-23-0453

CD106 in Tumor-Specific Exhausted CD8+ T Cells Mediates Immunosuppression by Inhibiting TCR Signaling

Yuto Naoi(Okayama University), Takao Morinaga(Chiba Cancer Center), Joji Nagasaki(Okayama University), Ryo Ariyasu(National Cancer Center Hospital East), Youki Ueda(Okayama University), Kazuo Yamashita(TagCyx Biotechnologies (Japan)), Wenhao Zhou(Okayama University), Shusuke Kawashima(Chiba University), Katsushige Kawase(Chiba University), Akiko Honobe‐Tabuchi(University of Yamanashi), Takehiro Ohnuma(University of Yamanashi), Tatsuyoshi Kawamura(University of Yamanashi), Yoshiyasu Umeda(Saitama Medical University), Yu Kawahara(Chiba University), Yasuhiro Nakamura(Saitama Medical University), Yukiko Kiniwa(Shinshu University), Osamu Yamasaki(Okayama University), Satoshi Fukushima(Kumamoto University), Masahito Kawazu(Chiba Cancer Center), Yutaka Suzuki(Chiba University), Hiroyoshi Nishikawa(National Cancer Center Hospital East), Toyoyuki Hanazawa(Chiba University), Mizuo Ando(Okayama University), Takashi Inozume(Chiba University), Yosuke Togashi(Okayama University)

Cancer Research

April 18, 2024

10.1158/0008-5472.can-23-0453

Cited by 10

Abstract

T-cell exhaustion is a major contributor to immunosuppression in the tumor microenvironment (TME). Blockade of key regulators of T-cell exhaustion, such as programmed death 1, can reinvigorate tumor-specific T cells and activate antitumor immunity in various types of cancer. In this study, we identified that CD106 was specifically expressed in exhausted CD8+ T cells in the TME using single-cell RNA sequencing. High CD106 expression in the TME in clinical samples corresponded to improved response to cancer immunotherapy. CD106 in tumor-specific T cells suppressed antitumor immunity both in vitro and in vivo, and loss of CD106 in CD8+ T cells suppressed tumor growth and improved response to programmed death 1 blockade. Mechanistically, CD106 inhibited T-cell receptor (TCR) signaling by interacting with the TCR/CD3 complex and reducing its surface expression. Together, these findings provide insights into the immunosuppressive role of CD106 expressed in tumor-specific exhausted CD8+ T cells, identifying it as a potential biomarker and therapeutic target for cancer immunotherapy. Significance: CD106 is specifically expressed in tumor-specific exhausted CD8+ T cells and inhibits the TCR signaling pathway by reducing surface expression of the TCR/CD3 complex to suppress antitumor immunity.

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