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首页> 外文期刊>The journal of immunology >Expression Hierarchy of T Cell Epitopes from Melanoma Differentiation Antigens: Unexpected High Level Presentation of Tyrosinase-HLA-A2 Complexes Revealed by Peptide-Specific, MHC-Restricted, TCR-Like Antibodies
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Expression Hierarchy of T Cell Epitopes from Melanoma Differentiation Antigens: Unexpected High Level Presentation of Tyrosinase-HLA-A2 Complexes Revealed by Peptide-Specific, MHC-Restricted, TCR-Like Antibodies

机译:黑色素瘤分化抗原的T细胞表位的表达层次:酪氨酸酶-HLA-A2复杂的意外高水平呈现肽特异性,MHC限制,TCR样抗体揭示。

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Peptide Ags presented by class I MHC molecules on human melanomas and that are recognized by CD8+ T cells are the subjects of many studies of antitumor immunity and represent attractive candidates for therapeutic approaches. However, no direct quantitative measurements exist to reveal their expression hierarchy on the cell surface. Using novel recombinant Abs which bind these Ags with a peptide-specific, MHC-restricted manner, we demonstrate a defined pattern of expression hierarchy of peptide-HLA-A2 complexes derived from three major differentiation Ags: gp100, Melan-A/Mart-1, and tyrosinase. Studying melanoma cell lines derived from multiple patients, we reveal a surprisingly high level of presentation of tyrosinase-derived complexes and moderate to very low expression of complexes derived from other Ags. No correlation between Ag presentation and mRNA expression was found; however, protein stability may play a major role. These results provide new insights into the characteristics of Ag presentation and are particularly important when such targets are being considered for immunotherapy. These results may shed new light on relationships between Ag presentation and immune response to cancer Ags.
机译:由I类MHC分子呈递给人类黑色素瘤并被CD8 + T细胞识别的肽Ags是许多抗肿瘤免疫研究的主题,是治疗方法的诱人候选物。但是,不存在直接的定量测量来揭示它们在细胞表面的表达层次。使用新颖的重组Abs以肽特异性,MHC限制的方式结合这些Ags,我们证明了衍生自三种主要分化Ags:gp100,Melan-A / Mart-1的肽-HLA-A2复合物的表达层次结构的定义模式和酪氨酸酶。研究来自多个患者的黑色素瘤细胞系,我们发现酪氨酸酶衍生的复合物表现出令人惊讶的高水平表达,而来自其他Ags的复合物的表达则处于中等至极低的水平。没有发现抗原呈递与mRNA表达之间的相关性;但是,蛋白质稳定性可能起主要作用。这些结果提供了有关Ag呈递特征的新见解,并且在考虑将此类靶标用于免疫治疗时尤其重要。这些结果可能为抗原呈递与对癌症抗原的免疫反应之间的关系提供新的启示。

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