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首页> 外文期刊>Clinical and vaccine immunology: CVI >Neem leaf glycoprotein partially rectifies suppressed dendritic cell functions and associated T cell efficacy in patients with stage IIIB cervical cancer.
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Neem leaf glycoprotein partially rectifies suppressed dendritic cell functions and associated T cell efficacy in patients with stage IIIB cervical cancer.

机译:印楝叶糖蛋白部分矫正和抑制树突状细胞功能患者T细胞功效相关的阶段希望子宫颈癌。

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Myeloid-derived dendritic cells (DCs) generated from monocytes obtained from stage IIIB cervical cancer (CaCx IIIB) patients show dysfunctional maturation; thus, antitumor T cell functions are dysregulated. In an objective to optimize these dysregulated immune functions, the present study is focused on the ability of neem leaf glycoprotein (NLGP), a nontoxic preparation of the neem leaf, to induce optimum maturation of dendritic cells from CaCx IIIB patients. In vitro NLGP treatment of immature DCs (iDCs) obtained from CaCx IIIB patients results in upregulated expression of various cell surface markers (CD40, CD83, CD80, CD86, and HLA-ABC), which indicates DC maturation. Consequently, NLGP-matured DCs displayed balanced cytokine secretions, with type 1 bias and noteworthy functional properties. These DCs displayed substantial T cell allostimulatory capacity and promoted the generation of cytotoxic T lymphocytes (CTLs). Although NLGP-matured DCs derived from CaCx monocytes are generally subdued compared to those with a healthy monocyte origin, considerable revival of the suppressed DC-based immune functions is noted in vitro at a fairly advanced stage of CaCx, and thus, further exploration of ex vivo and in vivo DC-based vaccines is proposed. Moreover, the DC maturating efficacy of NLGP might be much more effective in the earlier stages of CaCx, where the extent of immune dysregulation is less and, thus, the scope of further investigation may be explored.
机译:Myeloid-derived树突状细胞(dc)生成的从单核细胞获得阶段希望具有颈癌症(CaCx希望)患者显示不正常成熟;特异表达。特异表达的免疫功能,目前的研究重点是印楝叶的能力吗糖蛋白(NLGP),无毒的准备印楝叶,诱导最佳成熟树突细胞从CaCx希望病人。NLGP治疗未成熟dc (idc)获得从CaCx希望病人结果调节各种细胞表面标记物的表达(CD40,CD83、CD80、CD86和HLA-ABC),这表明DC成熟。显示平衡细胞因子分泌,类型1偏见和值得注意的功能性质。这些DCs显示大量的T细胞allostimulatory容量和促进了一代的细胞毒性T淋巴细胞(ctl)。尽管来自CaCx NLGP-matured DCs单核细胞一般柔和相比与健康的单核细胞起源,可观位于抑制免疫的复兴函数指出体外相当先进CaCx的阶段,因此,进一步的探索体外和体内的华盛顿疫苗建议。早些时候NLGP可能更有效CaCx阶段,免疫的程度失调更少,因此,的范围进一步研究可以探索。

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