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β‐Glucan enhances antitumor immune responses by regulating differentiation and function of monocytic myeloid‐derived suppressor cells
Authors:Jie Tian  Jie Ma  Ke Ma  Hongye Guo  Samuel Essien Baidoo  Yue Zhang  Jun Yan  Liwei Lu  Huaxi Xu  Shengjun Wang
Affiliation:1. Department of Laboratory Medicine, The Affiliated People's Hospital, Jiangsu University School of Medical Science and Laboratory Medicine, , Zhenjiang, China;2. Institute of Laboratory Medicine, Jiangsu University, , Zhenjiang, China;3. Tumor Immunobiology Program, James Graham Brown Cancer Center, University of Louisville, , KY, USA;4. Department of Pathology and Centre of Infection and Immunology, The University of Hong Kong, , Hong Kong, China
Abstract:Myeloid‐derived suppressor cells (MDSCs) accumulate in tumor‐bearing hosts and play a major role in tumor‐induced immunosuppression, which hampers effective immuno‐therapeutic approaches. β‐Glucans have been reported to function as potent immuno‐modulators to stimulate innate and adaptive immune responses, which contributes to their antitumor property. Here, we investigated the effect of particulate β‐glucans on MDSCs and found that β‐glucan treatment could promote the differentiation of M‐MDSCs (monocytic MDSCs) into a more mature CD11c+ F4/80+ Ly6Clow population via dectin‐1 pathway in vitro, which is NF‐κB dependent, and the suppressive function of M‐MDSCs was significantly decreased. Treatment of orally administered yeast‐derived particulate β‐glucan drastically downregulated MDSCs but increased the infiltrated DCs and macrophages in tumor‐bearing mice, thus eliciting CTL and Th1 responses, inhibiting the suppressive activity of regulatory T cells, thereby leading to the delayed tumor progression. We show here for the first time that β‐glucans induce the differentiation of MDSCs and inhibit the regulatory function of MDSCs, therefore revealing a novel mechanism for β‐glucans in immunotherapy and suggesting their potential clinical benefit.
Keywords:Dectin‐1  Dendritic cells  β  ‐Glucan  Myeloid‐derived suppressor cells  Tumor immunotherapy
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