Recognition of naturally processed and ovarian cancer reactive CD8+ T cell epitopes within a promiscuous HLA class II T-helper region of NY-ESO-1

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作者
Junko Matsuzaki
Feng Qian
Immanuel Luescher
Shashikant Lele
Gerd Ritter
Protul A. Shrikant
Sacha Gnjatic
Lloyd J. Old
Kunle Odunsi
机构
[1] Roswell Park Cancer Institute,Departments of Gynecologic Oncology and Immunology
[2] Ludwig Institute for Cancer Research,Department of Gynecologic Oncology
[3] Roswell Park Cancer Institute,New York Branch at Memorial Sloan
[4] Ludwig Institute for Cancer Research,Kettering Cancer Center
[5] Roswell Park Cancer Institute,Department of Immunology
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关键词
Epithelial ovarian cancer; Tumor immunity; NY-ESO-1; CD8; Epitope; MHC class I;
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摘要
NY-ESO-1 is frequently expressed in epithelial ovarian cancer (EOC) and elicits spontaneous humoral and cellular immune responses in a proportion of EOC patients. The identification of NY-ESO-1 peptide epitopes with dual HLA-class I and class II specificities might be useful in vaccination strategies for generating cognate CD4+ T cell help to augment CD8+ T cell responses. Here, we describe two novel NY-ESO-1-derived MHC class I epitopes from EOC patients with spontaneous humoral immune response to NY-ESO-1. CD8+ T cells derived from NY-ESO-1 seropositive EOC patients were presensitized with a recombinant adenovirus encoding NY-ESO-1or pooled overlapping peptides. These epitopes, ESO127–136 presented by HLA-A68 molecule, and ESO127–135 restricted by HLA-Cw15 allele, are located within ESO119–143, a promiscuous HLA-class II region containing epitopes that bind to multiple HLA-DR alleles. The novel epitopes were naturally processed by APC or naturally presented by tumor cell lines. In addition, these epitopes induced NY-ESO-1-specific CTL in NY-ESO-1 seropositive EOC patients. Together, the results indicate that ESO119–143 epitope has dual HLA classes I and II specificities, and represents a potential vaccine candidate in a large number of cancer patients.
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页码:1185 / 1195
页数:10
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