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Myeloid-derived suppressor cell function is reduced by Withaferin A, a potent and abundant component of Withania somnifera root extract

机译:用含有素A,含量和丰富的含有丰富的含有丰富的含量和丰富的组分减少了骨髓衍生的抑制细胞功能

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Myeloid cells play a crucial role in tumor progression. The most common tumor-infiltrating myeloid cells are myeloid-derived suppressor cells (MDSC) and tumor-associated macrophages (TAMs). These cells promote tumor growth by their inherent immune suppressive activity which is enhanced by their cross-talk. The root extract of the plant Withania somnifera (Ashwagandha) (WRE) has been reported to reduce tumor growth. HPLC analysis identified Withaferin A (WA) as the most abundant constituent of WRE and led us to determine whether the anti-tumor effects of WRE and WA involve modulating MDSC and TAM activity. A prominent effect of MDSC is their production of IL-10 which increases upon cross-talk with macrophages, thus polarizing immunity to a pro-tumor type 2 phenotype. In vitro treatment with WA decreased MDSC production of IL-10 and prevented additional MDSC production of IL-10 generated by MDSC-macrophage cross-talk. Macrophage secretion of IL-6 and TNFα, cytokines that increase MDSC accumulation and function, was also reduced by in vitro treatment with WA. Much of the T-cell suppressive activity of MDSC is due to MDSC production of reactive oxygen species (ROS), and WA significantly reduced MDSC production of ROS through a STAT3-dependent mechanism. In vivo treatment of tumor-bearing mice with WA decreased tumor weight, reduced the quantity of granulocytic MDSC, and reduced the ability of MDSC to suppress antigen-driven activation of CD4 + and CD8+ T cells. Thus, adjunctive treatment with WA reduced myeloid cell-mediated immune suppression, polarized immunity toward a tumor-rejecting type 1 phenotype, and may facilitate the development of anti-tumor immunity.
机译:骨髓细胞在肿瘤进展中发挥着至关重要的作用。最常见的肿瘤渗透髓样细胞是骨髓衍生的抑制细胞(MDSC)和肿瘤相关的巨噬细胞(TAMS)。这些细胞通过其固有的免疫抑制活性促进肿瘤生长,其通过其串扰增强。据报道,植物植物的根提取物(Ashwagandha)(WHE)以降低肿瘤生长。 HPLC分析鉴定为Wreferin A(WA)作为WRE最丰富的组成,并导致我们确定WRE和WA的抗肿瘤作用是否涉及调节MDSC和TAM活性。 MDSC的突出效果是它们的IL-10生产,其在牛话与巨噬细胞串扰时增加,从而使免疫偏振于促肿瘤2种表型。用WA的体外处理减少IL-10的MDSC生产,并防止了MDSC-巨噬细胞串扰产生的IL-10的额外MDSC生产。通过用Wa体外处理,还减少了IL-6和TNFα的巨噬细胞分泌,细胞因子增加了MDSC积聚和功能。 MDSC的大部分T细胞抑制活性是由于MDSC产生反应性氧物质(ROS),并且WA通过STAT3依赖性机制显着降低了ROS的MDSC生产。体内用WA减少肿瘤重量瘤小鼠的肿瘤小鼠,降低了粒细胞MDSC的量,降低了MDSC抑制CD4 +和CD8 + T细胞的抗原驱动活化的能力。因此,用VA的辅助治疗减少骨髓细胞介导的免疫抑制,朝向肿瘤排斥的1型表型的偏振免疫,并且可以促进抗肿瘤免疫的发展。

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