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B lymphocytes as direct antigen-presenting cells for anti-tumor DNA vaccines

机译:B淋巴细胞作为抗肿瘤DNA疫苗的直接抗原呈递细胞

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摘要

In spite of remarkable preclinical efficacy, DNA vaccination has demonstrated low immunogenicity in humans. While efforts have focused on increasing cross-presentation of DNA-encoded antigens, efforts to increase DNA vaccine immunogenicity by targeting direct presentation have remained mostly unexplored. In these studies, we compared the ability of different APCs to present antigen to T cells after simple co-culture with plasmid DNA. We found that human primary peripheral B lymphocytes, and not monocytes or in vitro derived dendritic cells (DCs), were able to efficiently encode antigen mRNA and expand cognate tumor antigen-specific CD8 T cells ex vivo. Similarly, murine B lymphocytes co-cultured with plasmid DNA, and not DCs, were able to prime antigen-specific T cells in vivo. Moreover, B lymphocyte-mediated presentation of plasmid antigen led to greater Th1-biased immunity and was sufficient to elicit an anti-tumor effect in vivo. Surprisingly, increasing plasmid presentation by B cells, and not cross presentation of peptides by DCs, further augmented traditional plasmid vaccination. Together, these data suggest that targeting plasmid DNA to B lymphocytes, for example through transfer of ex vivo plasmidloaded B cells, may be novel means to achieve greater T cell immunity from DNA vaccines.
机译:尽管临床前疗效显着,但DNA疫苗接种已证明对人体具有较低的免疫原性。尽管努力集中在增加DNA编码抗原的交叉展示上,但通过靶向直接呈递提高DNA疫苗免疫原性的努力仍未开发。在这些研究中,我们比较了与质粒DNA简单共培养后不同APC向T细胞呈递抗原的能力。我们发现人类原发性外周血B淋巴细胞,而不是单核细胞或体外衍生的树突状细胞(DC),能够有效编码抗原mRNA,并离体扩增同源肿瘤抗原特异性CD8 T细胞。同样,与质粒DNA共培养的鼠B淋巴细胞,而不与DC共培养,能够在体内引发抗原特异性T细胞。此外,B淋巴细胞介导的质粒抗原的呈递导致更大的Th1偏向免疫力,足以在体内引起抗肿瘤作用。出乎意料的是,增加了B细胞的质粒呈递,而不是DC的肽交叉呈递,进一步增加了传统的质粒疫苗接种。总之,这些数据表明,例如通过转移离体质粒加载的B细胞,将质粒DNA靶向B淋巴细胞,可能是从DNA疫苗中获得更大T细胞免疫力的新颖手段。

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