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首页> 外文期刊>Cancer letters >Adjuvant effect of a natural TLR4 ligand on dendritic cell-based cancer immunotherapy.
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Adjuvant effect of a natural TLR4 ligand on dendritic cell-based cancer immunotherapy.

机译:天然TLR4配体对基于树突细胞的癌症免疫治疗的辅助作用。

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The clinical efficacy of dendritic cell (DC) vaccine in cancer patients has been unsatisfactory due, at least in part, to the deficiency of maturation and impaired migration of ex vivo generated DCs to the draining lymph nodes. To solve this problem, we used angelan, a natural TLR4 ligand, to enhance the maturation and migration of DCs. Angelan increased the expression of MHC-I/II, CD80, and CD86, DC maturation markers, through the NF-kappaB pathway. This compound also increased CCR7 expression in DCs through NF-kappaB and p38 pathway and enhanced their migration against CCL19, which is a key chemokine that guides DCs into lymph nodes. We also showed that angelan enhanced in vivo DC homing from tissues to draining lymph nodes. When treated to DCs in vitro and vivo, angelan increased antitumor activity of DCs in B16F10 syngeneic tumor model. Taken together, the present data suggest that a natural TLR4 ligand might be helpful for overcoming the disadvantages of DC-based cancer therapy, such as impaired maturation and poor migration in cancer patients.
机译:树突状细胞(DC)疫苗在癌症患者中的临床疗效一直不令人满意,至少部分原因是缺乏成熟度以及离体产生的DC到引流淋巴结的迁移受到损害。为了解决此问题,我们使用了天然的TLR4配体angelan来增强DC的成熟和迁移。 Angelan通过NF-κB途径增加了MHC-I / II,CD80和CD86,DC成熟标记的表达。该化合物还通过NF-κB和p38途径增加了DC中CCR7的表达,并增强了其针对CCL19的迁移,CCL19是引导DC进入淋巴结的关键趋化因子。我们还表明,安吉兰增强了从组织到引流淋巴结的体内DC归巢。当在体外和体内对DC进行治疗时,当归在B16F10同基因肿瘤模型中增加DC的抗肿瘤活性。综上所述,目前的数据表明,天然的TLR4配体可能有助于克服基于DC的癌症治疗方法的弊端,例如成熟度降低和癌症患者迁移不良。

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