| Literature DB >> 34103370 |
Wei X Huff1, Marpe Bam2, Jack M Shireman2, Jae Hyun Kwon1, Leo Song1, Sharlé Newman1, Aaron A Cohen-Gadol1, Scott Shapiro1, Tamara Jones3, Kelsey Fulton3, Sheng Liu3, Hiromi Tanaka3, Yunlong Liu3, Jun Wan3, Mahua Dey4.
Abstract
Clinical use of various forms of immunotherapeutic drugs in glioblastoma (GBM), has highlighted severe T cell dysfunction such as exhaustion in GBM patients. However, reversing T cell exhaustion using immune checkpoint inhibitors in GBM clinical trials has not shown significant overall survival benefit. Phenotypically, CD8+ T cells with downregulated CD28 coreceptors, low CD27 expression, increased CD57 expression, and telomere shortening are classified as senescent T cells. These senescent T cells are normally seen as part of aging and also in many forms of solid cancers. Absence of CD28 on T cells leads to several functional irregularities including reduced TCR diversity, incomplete activation of T cells, and defects in Ag-induced proliferation. In the context of GBM, presence and/or function of these CD8+CD28- T cells is unknown. In this clinical correlative study, we investigated the effect of aging as well as tumor microenvironment on CD8+ T cell phenotype as an indicator of its function in GBM patients. We systematically analyzed and describe a large population of CD8+CD28- T cells in both the blood and tumor-infiltrating lymphocytes of GBM patients. We found that phenotypically these CD8+CD28- T cells represent a distinct population compared with exhausted T cells. Comparative transcriptomic and pathway analysis of CD8+CD28- T cell populations in GBM patients revealed that tumor microenvironment might be influencing several immune related pathways and thus further exaggerating the age associated immune dysfunction in this patient population.Entities:
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Year: 2021 PMID: 34103370 PMCID: PMC8591704 DOI: 10.4049/immunohorizons.2100008
Source DB: PubMed Journal: Immunohorizons ISSN: 2573-7732