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TIGIT/CD155 axis mediates resistance to immunotherapy in patients with melanoma with the inflamed tumor microenvironment.
Kawashima, Shusuke; Inozume, Takashi; Kawazu, Masahito; Ueno, Toshihide; Nagasaki, Joji; Tanji, Etsuko; Honobe, Akiko; Ohnuma, Takehiro; Kawamura, Tatsuyoshi; Umeda, Yoshiyasu; Nakamura, Yasuhiro; Kawasaki, Tomonori; Kiniwa, Yukiko; Yamasaki, Osamu; Fukushima, Satoshi; Ikehara, Yuzuru; Mano, Hiroyuki; Suzuki, Yutaka; Nishikawa, Hiroyoshi; Matsue, Hiroyuki; Togashi, Yosuke.
Afiliação
  • Kawashima S; Research Institute, Chiba Cancer Center, Chiba, Japan.
  • Inozume T; Department of Dermatology, Chiba University Graduate School of Medicine, Chiba, Japan.
  • Kawazu M; Research Institute, Chiba Cancer Center, Chiba, Japan.
  • Ueno T; Department of Dermatology, Chiba University Graduate School of Medicine, Chiba, Japan.
  • Nagasaki J; Department of Dermatology, University of Yamanashi, Chuo, Japan.
  • Tanji E; Research Institute, Chiba Cancer Center, Chiba, Japan.
  • Honobe A; Division of Cellular Signaling, National Cancer Center Research Institute, Chuo-ku, Japan.
  • Ohnuma T; Division of Cellular Signaling, National Cancer Center Research Institute, Chuo-ku, Japan.
  • Kawamura T; Research Institute, Chiba Cancer Center, Chiba, Japan.
  • Umeda Y; Research Institute, Chiba Cancer Center, Chiba, Japan.
  • Nakamura Y; Department of Dermatology, University of Yamanashi, Chuo, Japan.
  • Kawasaki T; Department of Dermatology, University of Yamanashi, Chuo, Japan.
  • Kiniwa Y; Department of Dermatology and Plastic Surgery, Faculty of Life Sciences, Kumamoto University, Kumamoto, Japan.
  • Yamasaki O; Department of Dermatology, University of Yamanashi, Chuo, Japan.
  • Fukushima S; Department of Skin Oncology/Dermatology, Saitama Medical University International Medical Center, Hidaka, Japan.
  • Ikehara Y; Department of Skin Oncology/Dermatology, Saitama Medical University International Medical Center, Hidaka, Japan.
  • Mano H; Department of Pathology, Saitama Medical University International Medical Center, Hidaka, Japan.
  • Suzuki Y; Department of Dermatology, Shinshu University School of Medicine, Matsumoto, Japan.
  • Nishikawa H; Department of Dermatology, Okayama University Graduate School of Medicine, Dentistry and Pharmaceutical Sciences, Okayama, Japan.
  • Matsue H; Department of Dermatology and Plastic Surgery, Faculty of Life Sciences, Kumamoto University, Kumamoto, Japan.
  • Togashi Y; Department of Molecular and Tumor Pathology, Chiba University Graduate School of Medicine, Chiba, Japan.
J Immunother Cancer ; 9(11)2021 11.
Article em En | MEDLINE | ID: mdl-34795004
ABSTRACT

BACKGROUND:

Patients with cancer benefit from treatment with immune checkpoint inhibitors (ICIs), and those with an inflamed tumor microenvironment (TME) and/or high tumor mutation burden (TMB), particularly, tend to respond to ICIs; however, some patients fail, whereas others acquire resistance after initial response despite the inflamed TME and/or high TMB. We assessed the detailed biological mechanisms of resistance to ICIs such as programmed death 1 and/or cytotoxic T-lymphocyte-associated protein 4 blockade therapies using clinical samples.

METHODS:

We established four pairs of autologous tumor cell lines and tumor-infiltrating lymphocytes (TILs) from patients with melanoma treated with ICIs. These tumor cell lines and TILs were subjected to comprehensive analyses and in vitro functional assays. We assessed tumor volume and TILs in vivo mouse models to validate identified mechanism. Furthermore, we analyzed additional clinical samples from another large melanoma cohort.

RESULTS:

Two patients were super-responders, and the others acquired resistance the first patient had a non-inflamed TME and acquired resistance due to the loss of the beta-2 microglobulin gene, and the other acquired resistance despite having inflamed TME and extremely high TMB which are reportedly predictive biomarkers. Tumor cell line and paired TIL analyses showed high CD155, TIGIT ligand, and TIGIT expression in the tumor cell line and tumor-infiltrating T cells, respectively. TIGIT blockade or CD155-deletion activated T cells in a functional assay using an autologous cell line and paired TILs from this patient. CD155 expression increased in surviving tumor cells after coculturing with TILs from a responder, which suppressed TIGIT+ T-cell activation. Consistently, TIGIT blockade or CD155-deletion could aid in overcoming resistance to ICIs in vivo mouse models. In clinical samples, CD155 was related to resistance to ICIs in patients with melanoma with an inflamed TME, including both primary and acquired resistance.

CONCLUSIONS:

The TIGIT/CD155 axis mediates resistance to ICIs in patients with melanoma with an inflamed TME, promoting the development of TIGIT blockade therapies in such patients with cancer.
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Texto completo: 1 Bases de dados: MEDLINE Assunto principal: Receptores Virais / Receptores Imunológicos / Imunoterapia / Melanoma Tipo de estudo: Prognostic_studies Limite: Aged / Animals / Female / Humans / Male Idioma: En Revista: J Immunother Cancer Ano de publicação: 2021 Tipo de documento: Article País de afiliação: Japão
Texto completo
Adicionar na Minha BVS
Imprimir
XML
PubMed Links
Buscar no Google

Texto completo: 1 Bases de dados: MEDLINE Assunto principal: Receptores Virais / Receptores Imunológicos / Imunoterapia / Melanoma Tipo de estudo: Prognostic_studies Limite: Aged / Animals / Female / Humans / Male Idioma: En Revista: J Immunother Cancer Ano de publicação: 2021 Tipo de documento: Article País de afiliação: Japão