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内在的哨兵:利用免疫系统寻找癌症生物标志物。

The sentinel within: exploiting the immune system for cancer biomarkers.

作者信息

Anderson Karen S, LaBaer Joshua

机构信息

Dana-Farber Cancer Institute, Harvard Medical School, Boston, MA 02115, USA.

出版信息

J Proteome Res. 2005 Jul-Aug;4(4):1123-33. doi: 10.1021/pr0500814.

Abstract

The release of proteins from tumors triggers an immune response in cancer patients. These tumor antigens arise from several mechanisms including tumor-specific alterations in protein expression, mutation, folding, degradation, or intracellular localization. Responses to most tumor antigens are rarely observed in healthy individuals, making the response itself a biomarker that betrays the presence of underlying cancer. Antibody immune responses show promise as clinical biomarkers because antibodies have long half-lives in serum, are easy to measure, and are stable in blood samples. However, our understanding of the specificity and the impact of the immune response in early stages of cancer is limited. The immune response to cancer, whether endogenous or driven by vaccines, involves highly specific T lymphocytes (which target tumor-derived peptides bound to self-MHC proteins) and B lymphocytes (which generate antibodies to tumor-derived proteins). T cell target antigens have been identified either by expression cloning from tumor cDNA libraries, or by prediction based on patterns of antigen expression ("reverse immunology"). B cell targets have been similarly identified using the antibodies in patient sera to screen cDNA libraries derived from tumor cell lines. This review focuses on the application of recent advances in proteomics for the identification of tumor antigens. These advances are opening the door for targeted vaccine development, and for using immune response signatures as biomarkers for cancer diagnosis and monitoring.

摘要

肿瘤释放的蛋白质会引发癌症患者的免疫反应。这些肿瘤抗原产生于多种机制,包括蛋白质表达、突变、折叠、降解或细胞内定位的肿瘤特异性改变。在健康个体中很少观察到对大多数肿瘤抗原的反应,因此这种反应本身成为了一种揭示潜在癌症存在的生物标志物。抗体免疫反应有望成为临床生物标志物,因为抗体在血清中的半衰期长、易于测量且在血样中稳定。然而,我们对癌症早期免疫反应的特异性及其影响的了解有限。对癌症的免疫反应,无论是内源性的还是由疫苗驱动的,都涉及高度特异性的T淋巴细胞(靶向与自身MHC蛋白结合的肿瘤衍生肽)和B淋巴细胞(产生针对肿瘤衍生蛋白的抗体)。T细胞靶抗原已通过从肿瘤cDNA文库中进行表达克隆或基于抗原表达模式的预测(“反向免疫学”)来鉴定。B细胞靶标也已通过使用患者血清中的抗体筛选源自肿瘤细胞系的cDNA文库来类似地鉴定。本综述重点关注蛋白质组学最新进展在肿瘤抗原鉴定中的应用。这些进展为靶向疫苗开发以及将免疫反应特征用作癌症诊断和监测的生物标志物打开了大门。

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