首页> 外文OA文献 >Activation of Tumor Antigen-Specific Cytotoxic T Lymphocytes (CTLs) by Human Dendritic Cells Infected with an Attenuated Influenza A Virus Expressing a CTL Epitope Derived from the HER-2/neu Proto-Oncogene
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Activation of Tumor Antigen-Specific Cytotoxic T Lymphocytes (CTLs) by Human Dendritic Cells Infected with an Attenuated Influenza A Virus Expressing a CTL Epitope Derived from the HER-2/neu Proto-Oncogene

机译:感染表达HER-2 / neu原癌基因CTL表位的减毒甲型流感病毒感染的人树突状细胞激活肿瘤抗原特异性细胞毒性T淋巴细胞(CTL)。

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摘要

The development of cancer vaccines requires approaches to induce expansion and functional differentiation of tumor antigen-specific cytotoxic T lymphocyte (CTL) effectors which posses cytolytic capability and produce cytokines. Efficient induction of such cells is hindered by the poor immunogenicity of tumor antigens and by the poor transduction efficiency of dendritic cells (DCs) with current nonreplicating vectors. We have investigated the use of influenza A virus, a potent viral inducer of CTLs, as a vector expressing the immunodominant HER-2 CTL epitope KIF (E75). For this purpose, an attenuated influenza A/PR8/34 virus with a truncated nonstructural (NS1) gene was generated containing the E75 epitope in its neuraminidase protein (KIF-NS virus). Stimulation of peripheral blood mononuclear cells from healthy donors and of tumor-associated lymphocytes from ovarian and breast cancer patients with DCs infected with KIF-NS virus (KIF-NS DC) induced CTLs that specifically recognized the peptide KIF and HER-2-expressing tumors in cytotoxicity assays and secreted gamma interferon (IFN-γ) and interleukin-2 at recall with peptide. Priming with KIF-NS DCs increased the number of E75+ CD45RO+ cells by more than 10-fold compared to nonstimulated cells. In addition, KIF-NS virus induced high levels of IFN-α in DCs. This is the first report demonstrating induction of human epitope-specific CTLs against a tumor-associated antigen with a live attenuated recombinant influenza virus vector. Such vectors may provide a novel approach for tumor antigen delivery, lymphocyte activation, and differentiation in human cancer vaccine development.
机译:癌症疫苗的开发需要诱导肿瘤抗原特异性细胞毒性T淋巴细胞(CTL)效应子的扩展和功能分化的方法,该效应子具有细胞溶解能力并产生细胞因子。肿瘤抗原的免疫原性差以及树突状细胞(DC)对当前非复制载体的转导效率差,阻碍了此类细胞的有效诱导。我们已经研究了使用甲型流感病毒(一种有效的CTL病毒诱导剂)作为表达具有免疫优势的HER-2 CTL表位KIF(E75)的载体的用途。为此,产生了具有截短的非结构性(NS1)基因的减毒A / PR8 / 34流感病毒,其神经氨酸酶蛋白中含有E75表位(KIF-NS病毒)。用KIF-NS病毒感染的DC刺激健康供体的外周血单核细胞以及卵巢癌和乳腺癌患者的肿瘤相关淋巴细胞(KIF-NS DC)诱导的CTL特异性识别肽KIF和HER-2表达的肿瘤在细胞毒性试验中的应用以及在召回肽时分泌的γ-干扰素(IFN-γ)和白介素-2。与未刺激的细胞相比,用KIF-NS DC引发的E75 + CD45RO +细胞数量增加了10倍以上。另外,KIF-NS病毒在DC中诱导高水平的IFN-α。这是第一份证明用减毒活的重组流感病毒载体诱导人表位特异性CTL对抗肿瘤相关抗原的报道。此类载体可为人类癌症疫苗开发中的肿瘤抗原递送,淋巴细胞活化和分化提供一种新颖的方法。

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