首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Commonly used prophylactic vaccines as an alternative for synthetically produced TLR ligands to mature monocyte-derived dendritic cells.
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Commonly used prophylactic vaccines as an alternative for synthetically produced TLR ligands to mature monocyte-derived dendritic cells.

机译:常用的预防性疫苗可以替代合成产生的TLR配体,替代成熟的单核细胞衍生的树突状细胞。

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摘要

Currently dendritic cell (DC)-based vaccines are explored in clinical trials, predominantly in cancer patients. Murine studies showed that only maturation with Toll-like receptor (TLR) ligands generates mature DCs that produce interleukin-12 and promote optimal T-cell help. Unfortunately, the limited availability of clinical-grade TLR ligands significantly hampers the translation of these findings into DC-based vaccines. Therefore, we explored 15 commonly used preventive vaccines as a possible source of TLR ligands. We have identified a cocktail of the vaccines BCG-SSI, Influvac, and Typhim that contains TLR ligands and is capable of optimally maturing DCs. These DCs (vaccine DCs) showed high expression of CD80, CD86, and CD83 and secreted interleukin-12. Although vaccine DCs exhibited an impaired migratory capacity, this could be restored by addition of prostaglandin E(2) (PGE(2); vaccine PGE(2) DCs). Vaccine PGE(2) DCs are potent inducers of T-cell proliferation and induce Th1 polarization. In addition, vaccine PGE(2) DCs are potent inducers of tumor antigen-specific CD8(+) effector T cells. Finally, vaccine PGE(2)-induced DC maturation is compatible with different antigen-loading strategies, including RNA electroporation. These data thus identify a new clinical application for a mixture of commonly used preventive vaccines in the generation of Th1-inducing clinical-grade mature DCs.
机译:目前,基于树突细胞(DC)的疫苗正在临床试验中进行探索,主要针对癌症患者。小鼠的研究表明,只有与Toll样受体(TLR)配体成熟,才能生成成熟的DC,这些DC产生白介素12并促进最佳的T细胞帮助。不幸的是,临床级TLR配体的有限可用性极大地阻碍了将这些发现转化为基于DC的疫苗。因此,我们探索了15种常用的预防性疫苗作为TLR配体的可能来源。我们已经确定了包含TLR配体并且能够最佳成熟DC的BCG-SSI,Influvac和Typhim疫苗的混合物。这些DC(疫苗DC)显示CD80,CD86和CD83的高表达并分泌白介素12。尽管疫苗DC表现出迁移能力受损,但可以通过添加前列腺素E(2)(PGE(2);疫苗PGE(2)DC)来恢复。疫苗PGE(2)DC是T细胞增殖的有效诱导剂,并诱导Th1极化。此外,疫苗PGE(2)DC是肿瘤抗原特异性CD8(+)效应T细胞的有效诱导剂。最后,疫苗PGE(2)诱导的DC成熟与不同的抗原加载策略(包括RNA电穿孔)兼容。因此,这些数据确定了常用的预防性疫苗混合物在诱导Th1的临床级成熟DC产生中的新临床应用。

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