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被人类T细胞识别的肿瘤特异性共享抗原肽。

Tumor-specific shared antigenic peptides recognized by human T cells.

作者信息

Van Der Bruggen Pierre, Zhang Yi, Chaux Pascal, Stroobant Vincent, Panichelli Christophe, Schultz Erwin S, Chapiro Jacques, Van Den Eynde Benoît J, Brasseur Francis, Boon Thierry

机构信息

Ludwig Institute for Cancer Research and Cellular Genetics Unit, Université de Louvain, 74 avenue Hippocrate UCL 74.59, B-1200 Brussels, Belgium.

出版信息

Immunol Rev. 2002 Oct;188:51-64. doi: 10.1034/j.1600-065x.2002.18806.x.

Abstract

The first tumor-specific shared antigens and the cancer-germline genes that code for these antigens were identified with antitumor cytolytic T lymphocytes obtained from cancer patients. A few HLA class I-restricted antigenic peptides were identified by this 'direct approach'. A large set of additional cancer-germline genes have now been identified by purely genetic approaches or by screening tumor cDNA expression libraries with the serum of cancer patients. As a result, a vast number of sequences are known that can code for tumor-specific shared antigens, but most of the encoded antigenic peptides have not yet been identified. We review here recent 'reverse immunology' approaches for the identification of new antigenic peptides. They are based on in vitro stimulation of naive T cells with dendritic cells that have either been loaded with a cancer-germline protein or that have been transduced with viruses carrying cancer-germline coding sequences. These approaches have led to the identification of many new antigenic peptides presented by class I or class II molecules. We also describe some aspects of the processing and presentation of these antigenic peptides.

摘要

利用从癌症患者体内获取的抗肿瘤细胞溶解T淋巴细胞,首次鉴定出了肿瘤特异性共享抗原以及编码这些抗原的癌胚基因。通过这种“直接方法”鉴定出了少数几种HLA I类限制性抗原肽。现在,通过纯遗传学方法或用癌症患者血清筛选肿瘤cDNA表达文库,又鉴定出了大量其他的癌胚基因。结果,已知大量能够编码肿瘤特异性共享抗原的序列,但大多数编码的抗原肽尚未被鉴定出来。在此,我们综述了近期用于鉴定新抗原肽的“反向免疫学”方法。这些方法基于用已负载癌胚蛋白的树突状细胞或用携带癌胚编码序列的病毒转导的树突状细胞,在体外刺激初始T细胞。这些方法已导致鉴定出许多由I类或II类分子呈递的新抗原肽。我们还描述了这些抗原肽加工和呈递的一些方面。

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