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Polarizing T and B Cell Responses by APC-Targeted Subunit Vaccines

机译:通过APC靶向亚单位疫苗极化T和B细胞反应

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摘要

Current influenza vaccines mostly aim at the induction of specific neutralizing antibodies. While antibodies are important for protection against a particular virus strain, T cells can recognize epitopes that will offer broader protection against influenza. We have previously developed a DNA vaccine format by which protein antigens can be targeted specifically to receptors on antigen presenting cells (APCs). The DNA-encoded vaccine proteins are homodimers, each chain consisting of a targeting unit, a dimerization unit, and an antigen. The strategy of targeting antigen to APCs greatly enhances immune responses as compared to non-targeted controls. Furthermore, targeting of antigen to different receptors on APCs can polarize the immune response to different arms of immunity. Here, we discuss how targeting of hemagglutinin to MHC class II molecules increases Th2 and IgG1 antibody responses, whereas targeting to chemokine receptors XCR1 or CCR1/3/5 increases Th1 and IgG2a responses, in addition to CD8+ T cell responses. We also discuss these results in relation to work published by others on APC-targeting. Differential targeting of APC surface molecules may allow the induction of tailor-made phenotypes of adaptive immune responses that are optimal for protection against various infectious agents, including influenza virus.
机译:当前的流感疫苗主要针对诱导特异性中和抗体。尽管抗体对于防御特定病毒株很重要,但T细胞可以识别可对流感提供更广泛保护的表位。我们以前已经开发出一种DNA疫苗形式,通过该形式,蛋白质抗原可以特异性地靶向抗原呈递细胞(APC)上的受体。 DNA编码的疫苗蛋白是同源二聚体,每条链均由靶向单元,二聚单元和抗原组成。与非靶向对照相比,将抗原靶向APC的策略大大增强了免疫反应。此外,将抗原靶向APC上的不同受体可以使针对不同免疫力的免疫反应极化。在这里,我们讨论了将血凝素靶向MHC II类分子如何增加Th2和IgG1抗体反应,而靶向趋化因子受体XCR1或CCR1 / 3/5除了CD8 + 之外如何增加Th1和IgG2a反应。 T细胞反应。我们还将讨论这些结果与其他人针对APC进行的工作有关。 APC表面分子的差异靶向可以诱导适应性免疫反应的特制表型,该表型对于保护抵抗包括流感病毒在内的各种传染原是最佳的。

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