Literature DB >> 21209773

T cells and stromal fibroblasts in human tumor microenvironments represent potential therapeutic targets.

Jennifer L Barnas1, Michelle R Simpson-Abelson, Sandra J Yokota, Raymond J Kelleher, Richard B Bankert.   

Abstract

The immune system of cancer patients recognizes tumor-associated antigens expressed on solid tumors and these antigens are able to induce tumor-specific humoral and cellular immune responses. Diverse immunotherapeutic strategies have been used in an attempt to enhance both antibody and T cell responses to tumors. While several tumor vaccination strategies significantly increase the number of tumor-specific lymphocytes in the blood of cancer patients, most vaccinated patients ultimately experience tumor progression. CD4+ and CD8+ T cells with an effector memory phenotype infiltrate human tumor microenvironments, but most are hyporesponsive to stimulation via the T cell receptor (TCR) and CD28 under conditions that activate memory T cells derived from the peripheral blood of the cancer patients or normal donors. Attempts to identify cells and molecules responsible for the TCR signaling arrest of tumor-infiltrating T cells have focused largely upon the immunosuppressive effects of tumor cells, tolerogenic dendritic cells and regulatory T cells. Here we review potential mechanisms by which human T cell function is arrested in the tumor microenvironment with a focus on the immunomodulatory effects of stromal fibroblasts. Determining in vivo which cells and molecules are responsible for the TCR arrest in human tumor-infiltrating T cells will be necessary to formulate and test strategies to prevent or reverse the signaling arrest of the human T cells in situ for a more effective design of tumor vaccines. These questions are now addressable using novel human xenograft models of tumor microenvironments.

Entities:  

Keywords:  Cancer; Fibroblast; Immunotherapy; Stromal cell; T lymphocyte; TCR signal transduction; Tumor microenvironment; Xenograft model

Year:  2010        PMID: 21209773      PMCID: PMC2990491          DOI: 10.1007/s12307-010-0044-5

Source DB:  PubMed          Journal:  Cancer Microenviron        ISSN: 1875-2284


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