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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Identification of new HER2eu-derived peptide epitopes that can elicit specific CTL against autologous and allogeneic carcinomas and melanomas.
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Identification of new HER2eu-derived peptide epitopes that can elicit specific CTL against autologous and allogeneic carcinomas and melanomas.

机译:鉴定新的HER2 / neu衍生的肽表位,可以引发针对自体和同种异体癌和黑色素瘤的特异性CTL。

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摘要

Twenty-two new HLA-A2.1-binding peptides derived from the protooncogene HER2eu were identified and analyzed for their capacity to elicit peptide and tumor-specific CTL responses. We used peptide-pulsed autologous DC from the ascites of patients with ovarian carcinomas to induce CTL. Of the 22 tested new HER2eu-derived epitopes that could bind HLA-A2 with high (IC50 < 50 nM) or intermediate (50 nM < IC50 < 500 nM) affinity, we report the recognition by CTL of at least four novel epitopes, including HER2(9435), HER2(9665), HER2(9689), and HER2(10952), and confirm that of the known HER2 (9369) epitope. These epitopes were able to elicit CTL that specifically killed peptide-sensitized target cells and, most importantly, a HER2eu-transfected cell line and the autologous tumor cells. We also confirm that HER2eu is overexpressed in several melanoma lines, and as a new finding, report that some of these lines are sensitive to CTL induced by the HER2 (9369), HER2(9435), and HER2(9689) epitopes. Finally, CTL clones specific for HER2 (9369), HER2(9435), and HER2(9689) epitopes were isolated from tumor-specific CTL lines, further demonstrating the immunodominance of these epitopes. These findings broaden the potential application of HER2eu-based immunotherapy.
机译:鉴定了来自原癌基因HER2 / neu的22种新的HLA-A2.1结合肽,并分析了它们引起肽和肿瘤特异性CTL应答的能力。我们使用来自卵巢癌患者腹水的肽脉冲自体DC诱导CTL。在22个经过测试的新HER2 / neu衍生表位中,它们可以以高(IC50 <50 nM)或中等(50 nM

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