首页> 外文期刊>The journal of immunology >Identification of BING-4 Cancer Antigen Translated From an Alternative Open Reading Frame of a Gene in the Extended MHC Class II Region Using Lymphocytes From a Patient With a Durable Complete Regression Following Immunotherapy
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Identification of BING-4 Cancer Antigen Translated From an Alternative Open Reading Frame of a Gene in the Extended MHC Class II Region Using Lymphocytes From a Patient With a Durable Complete Regression Following Immunotherapy

机译:使用来自免疫治疗后持久完全消退的患者的淋巴细胞,从扩展的MHC II类区域中的一个基因的替代开放阅读框架中鉴定出BING-4癌症抗原

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Multiple human cancer Ags have been identified, although little is known concerning which would be most effectively used in cancer immunotherapy. To gain insight into the selection of appropriate Ags, the immunologic reactivity of a patient who had a durable complete regression of melanoma metastases was measured. PBMCs were directly cloned using the monoclonal anti-CD3 Ab OKT3 and IL-2 without any bias introduced by previous culture. A lymphocyte clone recognized a previously unknown shared melanoma Ag that was identified as the BING-4 protein encoded in a gene-rich region of the extended class II MHC. The HLA-A2-restricted BING-4 immunodominant peptide was translated from a 10-aa-long alternative open reading frame. In vitro sensitization against this peptide generated lymphocytes reactive against HLA-A2+ melanomas. Real-time semiquantitative RT-PCR analysis revealed that 8 of 15 melanoma cell lines overexpressed BING-4, and this correlated with recognition by lymphocytes. Overexpression was not found in normal tissues or other tumor types. Thus, BING-4 represents another candidate Ag for possible use in the immunotherapy of patients with melanoma.
机译:已经鉴定出多种人类癌症抗原,尽管关于哪种抗原最有效地用于癌症免疫疗法的知之甚少。为了深入了解适当的Ags的选择,测量了黑色素瘤转移持续持久消退的患者的免疫反应性。使用单克隆抗CD3 Ab OKT3和IL-2直接克隆PBMC,而先前培养没有引入任何偏倚。淋巴细胞克隆识别出先前未知的共享黑色素瘤Ag,其被鉴定为在扩展的II类MHC的富含基因的区域中编码的BING-4蛋白。 HLA-A2限制性BING-4免疫优势肽是从10个氨基酸长的替代开放阅读框翻译而来的。对该肽的体外致敏作用产生了对HLA-A2 +黑色素瘤具有反应性的淋巴细胞。实时半定量RT-PCR分析显示,在15个黑色素瘤细胞系中有8个过表达BING-4,这与淋巴细胞的识别有关。在正常组织或其他肿瘤类型中未发现过表达。因此,BING-4代表了另一种可能用于黑色素瘤患者免疫治疗的候选抗原。

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