| Literature DB >> 34953280 |
David C Soler1, Amber Kerstetter-Fogle1, Andrew B Young2, Pat Rayman3, James H Finke3, Sarah M Debanne4, Kevin D Cooper2, Jill Barnholtz-Sloan5, Andrew E Sloan1, Thomas S McCormick6.
Abstract
Study of human monocytic Myeloid-Derived Suppressor cells Mo-MDSC (CD14+ HLA-DRneg/low) has been hampered by the lack of positive cell-surface markers. In order to identify positive markers for Mo-MDSC, we performed microarray analysis comparing Mo-MDSC cells from healthy subjects versus CD14+ HLA-DRhigh monocytes. We have identified the surface ectoenzyme Vanin-2(VNN2) protein as a novel biomarker highly-enriched in healthy subjects Mo-MDSC. Indeed, healthy subjects Mo-MDSC cells expressed 68 % VNN2, whereas only 9% VNN2 expression was observed on CD14+ HLA-DRhigh cells (n = 4 p < 0.01). The top 10 percent positive VNN2 monocytes expressed CD33 and CD11b while being negative for HLA-DR, CD3, CD15, CD19 and CD56, consistent with a Mo-MDSC phenotype. CD14+VNN2high monocytes were able to inhibit CD8 T cell proliferation comparably to traditional Mo-MDSC at 51 % and 48 % respectively. However, VNN2 expression on CD14+ monocytes from glioma patients was inversely correlated to their grade. CD14+VNN2high monocytes thus appear to mark a monocytic population similar to Mo-MDSC only in healthy subjects, which may be useful for tumor diagnoses.Entities:
Keywords: GPI-80; Immunosuppression; Mo-MDSC; VNN2
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Year: 2021 PMID: 34953280 PMCID: PMC8800381 DOI: 10.1016/j.molimm.2021.12.011
Source DB: PubMed Journal: Mol Immunol ISSN: 0161-5890 Impact factor: 4.407