| Literature DB >> 28344889 |
Yosuke Shionoya1, Takayuki Kanaseki2, Sho Miyamoto2, Serina Tokita2, Ayumi Hongo2, Yasuhiro Kikuchi2, Vitaly Kochin2, Kazue Watanabe3, Ryota Horibe1, Hiroshi Saijo1, Tomohide Tsukahara2, Yoshihiko Hirohashi2, Hiroki Takahashi4, Noriyuki Sato2, Toshihiko Torigoe2.
Abstract
Cytotoxic T-lymphocytes (CTLs) lyse target cells after recognizing the complexes of peptides and MHC class I molecules (pMHC I) on cell surfaces. Tapasin is an essential component of the peptide-loading complex (PLC) and its absence influences the surface repertoire of MHC class I peptides. In the present study, we assessed tapasin expression in 85 primary tumor lesions of non-small cell lung cancer (NSCLC) patients, demonstrating that tapasin expression positively correlated with patient survival. CD8+ T-cell infiltration of tumor lesions was synergistically observed with tapasin expression and correlated positively with survival. To establish a direct link between loss of tapasin and CTL recognition in human cancer models, we targeted the tapasin gene by CRISPR/Cas9 system and generated tapasin-deficient variants of human lung as well as colon cancer cells. We induced the CTLs recognizing endogenous tumor-associated antigens (TAA), survivin or cep55, and they responded to each tapasin-proficient wild type. In contrast, both CTL lines ignored the tapasin-deficient variants despite their antigen expression. Moreover, the adoptive transfer of the cep55-specific CTL line failed to prevent tumor growth in mice bearing the tapasin-deficient variant. Loss of tapasin most likely limited antigen processing of TAAs and led to escape from TAA-specific CTL recognition. Tapasin expression is thus a key for CTL surveillance against human cancers.Entities:
Keywords: CD8+ T cells; MHC class I; colon cancer; immune evasion; lung cancer; tapasin
Year: 2017 PMID: 28344889 PMCID: PMC5353923 DOI: 10.1080/2162402X.2016.1274476
Source DB: PubMed Journal: Oncoimmunology ISSN: 2162-4011 Impact factor: 8.110