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Erschienen in: Tumor Biology 1/2012

01.02.2012 | Research Article

CD15+/CD16low human granulocytes from terminal cancer patients: granulocytic myeloid-derived suppressor cells that have suppressive function

verfasst von: Jahyang Choi, Beomseok Suh, Yong-Oon Ahn, Tae Min Kim, Jeong-Ok Lee, Se-Hoon Lee, Dae Seog Heo

Erschienen in: Tumor Biology | Ausgabe 1/2012

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Abstract

Myeloid-derived suppressor cells (MDSCs) are a subpopulation of myeloid cells with immunosuppressive function whose numbers are increased in conditions such as chronic infection, trauma, and cancer. Unlike murine MDSCs defined as CD11b+/Gr-1+, there are no specific markers for human MDSCs. The goal of this study was to delineate a specific human MDSCs subpopulation in granulocytes from terminal cancer patients and investigate its clinical implications. Here, we show that the CD15+/CD16low subset was increased in terminal cancer patients compared with healthy donors (P = 0.009). Phorbol 12-myristate 13-acetate-activated granulocytes (CD16low/CD66b++/CD15+) that have a phenotype similar to MDSCs from cancer patients, effectively suppressed both proliferation and cytotoxicity of normal T cells. Among cancer patients, T-cell proliferation was highly suppressed by granulocytes isolated from terminal cancer patients with a high proportion of CD15+/CD16low cells. Patients with low peripheral blood levels of CD15+/CD16low cells had significantly longer survival than those with high levels (P = 0.0011). Patients with higher levels of CD15+/CD16low also tended to have poor performance status (P = 0.05). These data suggest that CD15+/CD16low granulocytes found in terminal cancer patients may play a role in the progression of cancer by inhibiting tumor immunity.
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Metadaten
Titel
CD15+/CD16low human granulocytes from terminal cancer patients: granulocytic myeloid-derived suppressor cells that have suppressive function
verfasst von
Jahyang Choi
Beomseok Suh
Yong-Oon Ahn
Tae Min Kim
Jeong-Ok Lee
Se-Hoon Lee
Dae Seog Heo
Publikationsdatum
01.02.2012
Verlag
Springer Netherlands
Erschienen in
Tumor Biology / Ausgabe 1/2012
Print ISSN: 1010-4283
Elektronische ISSN: 1423-0380
DOI
https://doi.org/10.1007/s13277-011-0254-6

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