| Literature DB >> 28768193 |
Hiroto Katoh1, Daisuke Komura1, Hiroki Konishi1, Ryohei Suzuki1, Asami Yamamoto1, Miwako Kakiuchi2, Reiko Sato1, Tetsuo Ushiku3, Shogo Yamamoto2, Kenji Tatsuno2, Takashi Oshima4, Sachiyo Nomura5, Yasuyuki Seto5, Masashi Fukayama3, Hiroyuki Aburatani2, Shumpei Ishikawa6.
Abstract
Recent successes in tumor immunotherapies have highlighted the importance of tumor immunity. However, most of the work conducted to date has been on T cell immunity, while the role of B cell immunity in cancer remains more elusive. In this study, immunogenetic repertoire profiling for tumor-infiltrating B and T cells in gastric cancers was carried out to help reveal the architecture of B cell immunity in cancer. Humoral immunity in cancer was shown to involve oligoclonal expansions of tumor-specific and private B cell repertoires. We find that B cell repertoires in cancer are shaped by somatic hypermutation (SHM) either with or without positive selection biases, the latter of which tended to be auto-reactive. Importantly, we identified sulfated glycosaminoglycans (GAGs) as major functional B cell antigens among gastric tumors. Furthermore, natural anti-sulfated GAG antibodies discovered in gastric cancer tissues showed robust growth-suppressive functions against a wide variety of human malignancies of various organs.Entities:
Keywords: gastric cancer; immunogenetics; repertoire sequence; sulfated glycosaminoglycan; therapeutic antibody; tumor immunity; tumor-infiltrating B cell
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Year: 2017 PMID: 28768193 DOI: 10.1016/j.celrep.2017.07.016
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423