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来自健康受试者和结肠癌患者的CD4(+) T细胞识别癌胚抗原特异性免疫显性表位。

CD4(+) T cells from healthy subjects and colon cancer patients recognize a carcinoembryonic antigen-specific immunodominant epitope.

作者信息

Campi Gabriele, Crosti Mariacristina, Consogno Giuseppe, Facchinetti Valeria, Conti-Fine Bianca M, Longhi Renato, Casorati Giulia, Dellabona Paolo, Protti Maria Pia

机构信息

Experimental Immunology Unit, Cancer Immunotherapy and Gene Therapy Program, Scientific Institute H. San Raffaele, 20132 Milan, Italy.

出版信息

Cancer Res. 2003 Dec 1;63(23):8481-6.

PMID:14679013
Abstract

The carcinoembryonic antigen (CEA) is an attractive target for immunotherapeutic purposes because of its expression profile, its role in tumor progression, and its immunogenicity. However, CEA belongs to the CD66 immunoglobulin super-gene family that comprises highly homologous molecules expressed on leukocytes, making CEA a potential autoantigen expressed on hematopoietic cells. We used a MHC class II epitope prediction algorithm (TEPITOPE) to select 11 sequence segments of CEA that could form promiscuous CD4(+) T-cell epitopes and used synthetic peptides corresponding to the predicted sequences to propagate in vitro CD4(+) T cells from healthy donors and colon cancer patients. CD4(+) T cells from all subjects strongly recognized the sequence segment (LWWVNNQSLPVSP), repeated at residues 177-189 and 355-367. Importantly, we demonstrated that this highly immunodominant region contains a naturally processed epitope(s). Cross-recognition experiments with peptide analogues present on the CD66 homologous proteins showed that CEA(177-189/355-367)-specific CD4(+) T cells did not recognize the analogues, demonstrating that recognition of the immunodominant epitope is CEA specific. These data suggest that the repertoire of CEA(177-189/355-367)-specific CD4(+) T cells might have been shaped by a selective process to exclude CD4(+) T cells specific for CD66 homologues expressed on leukocyte, while preserving the CEA-specific repertoire. The features of strong immunogenicity and immunodominance in the absence of potential induction of autoimmunity make the identified CEA epitope of particular interest for the development of antitumor vaccines.

摘要

癌胚抗原(CEA)因其表达谱、在肿瘤进展中的作用及其免疫原性,成为免疫治疗的一个有吸引力的靶点。然而,CEA属于CD66免疫球蛋白超基因家族,该家族包含在白细胞上表达的高度同源分子,这使得CEA成为造血细胞上潜在的自身抗原。我们使用一种II类主要组织相容性复合体(MHC)表位预测算法(TEPITOPE)来选择CEA的11个序列片段,这些片段可形成混杂的CD4(+) T细胞表位,并使用与预测序列对应的合成肽在体外扩增来自健康供体和结肠癌患者的CD4(+) T细胞。所有受试者的CD4(+) T细胞都强烈识别位于第177 - 189位和355 - 367位重复出现的序列片段(LWWVNNQSLPVSP)。重要的是,我们证明了这个高度免疫显性区域包含一个天然加工的表位。用CD66同源蛋白上存在的肽类似物进行的交叉识别实验表明,CEA(177 - 189/355 - 367)特异性CD4(+) T细胞不识别这些类似物,这表明对免疫显性表位的识别是CEA特异性的。这些数据表明,CEA(177 - 189/355 - 367)特异性CD4(+) T细胞库可能是通过一个选择性过程形成的,以排除对白细胞上表达的CD66同源物具有特异性的CD4(+) T细胞,同时保留CEA特异性库。在不存在自身免疫潜在诱导的情况下,其强大的免疫原性和免疫显性特征使得所鉴定的CEA表位在抗肿瘤疫苗开发中特别受关注。

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