HAGE,一种具有黑色素瘤免疫治疗潜力的癌胚抗原:几种MHC I/II类HAGE衍生免疫原性肽的鉴定。
HAGE, a cancer/testis antigen with potential for melanoma immunotherapy: identification of several MHC class I/II HAGE-derived immunogenic peptides.
作者信息
Mathieu Morgan G, Knights Ashley J, Pawelec Graham, Riley Catherine L, Wernet Dorothee, Lemonnier François A, Straten Per Thor, Mueller Ludmila, Rees Robert C, McArdle Stephanie E B
机构信息
School of Biomedical and Natural Science, Nottingham Trent University, Clifton Lane, Nottingham, NG11 8NS, UK.
出版信息
Cancer Immunol Immunother. 2007 Dec;56(12):1885-95. doi: 10.1007/s00262-007-0331-2. Epub 2007 May 9.
Abstract
There remains a need to identify novel epitopes of potential tumour target antigens for use in immunotherapy of cancer. Here, several melanoma tissues and cell lines but not normal tissues were found to overexpress the cancer-testis antigen HAGE at the mRNA and protein level. We identified a HAGE-derived 15-mer peptide containing a shorter predicted MHC class I-binding sequence within a class II-binding sequence. However, only the longer peptide was found to be both endogenously processed and immunogenic for T cells in transgenic mice in vivo, as well as for human T cells in vitro. A different class I-binding peptide, not contained within a longer class II sequence, was subsequently found to be both immunogenic and endogenously processed in transgenic mice, as was a second class II epitope. These novel HAGE-derived epitopes may contribute to the range of immunotherapeutic targets for use in cancer vaccination programs.
摘要
仍有必要鉴定潜在肿瘤靶抗原的新表位,以用于癌症免疫治疗。在此,发现几种黑色素瘤组织和细胞系而非正常组织在mRNA和蛋白质水平上过表达癌-睾丸抗原HAGE。我们鉴定出一种源自HAGE的15聚体肽,其在II类结合序列内含有较短的预测MHC I类结合序列。然而,仅发现较长的肽在体内转基因小鼠中以及在体外对人T细胞而言均可被内源性加工并具有免疫原性。随后发现一种不同的I类结合肽(其不包含在更长的II类序列内)以及第二个II类表位在转基因小鼠中均具有免疫原性且可被内源性加工。这些源自HAGE的新表位可能有助于扩大用于癌症疫苗接种计划的免疫治疗靶点范围。
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