| Literature DB >> 30628894 |
Daisuke Muraoka1,2,3, Naohiro Seo1,4, Tae Hayashi1, Yoshiro Tahara4,5,6, Keisuke Fujii1, Isao Tawara7, Yoshihiro Miyahara1, Kana Okamori1, Hideo Yagita8, Seiya Imoto9, Rui Yamaguchi10, Mitsuhiro Komura10, Satoru Miyano10, Masahiro Goto6, Shin-Ichi Sawada4,5, Akira Asai3, Hiroaki Ikeda2, Kazunari Akiyoshi4,5, Naozumi Harada1,4,11, Hiroshi Shiku1,4.
Abstract
Immune checkpoint inhibitors and adoptive transfer of gene-engineered T cells have emerged as novel therapeutic modalities for hard-to-treat solid tumors; however, many patients are refractory to these immunotherapies, and the mechanisms underlying tumor immune resistance have not been fully elucidated. By comparing the tumor microenvironment of checkpoint inhibition-sensitive and -resistant murine solid tumors, we observed that the resistant tumors had low immunogenicity. We identified antigen presentation by CD11b+F4/80+ tumor-associated macrophages (TAMs) as a key factor correlated with immune resistance. In the resistant tumors, TAMs remained inactive and did not exert antigen-presenting activity. Targeted delivery of a long peptide antigen to TAMs by using a nano-sized hydrogel (nanogel) in the presence of a TLR agonist activated TAMs, induced their antigen-presenting activity, and thereby transformed the resistant tumors into tumors sensitive to adaptive immune responses such as adoptive transfer of tumor-specific T cell receptor-engineered T cells. These results indicate that the status and function of TAMs have a significant impact on tumor immune sensitivity and that manipulation of TAM functions would be an effective approach for improving the efficacy of immunotherapies.Entities:
Keywords: Cancer immunotherapy; Immunology
Year: 2019 PMID: 30628894 PMCID: PMC6391090 DOI: 10.1172/JCI97642
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808