| Literature DB >> 27703529 |
Song Han1, Enlong Ma2, Xiaonan Wang2, Chunyong Yu1, Tao Dong1, Wen Zhan3, Xuezhong Wei1, Guobiao Liang1, Sizhe Feng1.
Abstract
Primary glioblastoma (GBM) is the most prevalent brain cancer, with fast progression and a poor prognosis. Current treatment options are unable to fully manage GBM since it is highly resistant to radiation and chemotherapy, and it cannot be completely removed by surgery. Thus, immunotherapeutic strategies utilizing tumor-infiltrating T cells have been investigated. In the present study, the T-cell response in GBM patients was examined in resected tumor samples and peripheral blood samples by flow cytometry. It was found that tumor-infiltrating T cells represented a rare population in all tumor cells, and were more refractory to anti-cluster of differentiation 3 (CD3) stimulation than their peripheral blood counterparts. A number of strategies were then assessed to boost tumor-infiltrating T-cell proliferation, and it was found that pre-incubation with 20 U/ml interleukin (IL)-2, as well as sequestration of IL-10 in culture, improved tumor T-cell proliferation following anti-CD3 stimulation. The stimulation of blood antigen-presenting cells by lipopolysaccharide, however, did not improve tumor T-cell proliferation. Overall, the present results provided a viable strategy for improving tumor-infiltrating CD3+ T-cell responses in GBM patients.Entities:
Keywords: IL-2; glioblastoma; tumor-infiltrating T-cell
Year: 2016 PMID: 27703529 PMCID: PMC5038909 DOI: 10.3892/ol.2016.4944
Source DB: PubMed Journal: Oncol Lett ISSN: 1792-1074 Impact factor: 2.967