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在表达MAGE-3基因的肿瘤细胞上由HLA-B44分子呈递的抗原肽的鉴定

Characterization of antigenic peptides presented by HLA-B44 molecules on tumor cells expressing the gene MAGE-3.

作者信息

Fleischhauer K, Fruci D, Van Endert P, Herman J, Tanzarella S, Wallny H J, Coulie P, Bordignon C, Traversari C

机构信息

Gene Therapy Program, Department of Biology and Biotechnology (DIBIT), Istituto Scientifico H.S. Raffaele, Milano, Italy.

出版信息

Int J Cancer. 1996 Nov 27;68(5):622-8. doi: 10.1002/(SICI)1097-0215(19961127)68:5<622::AID-IJC12>3.0.CO;2-3.

DOI:10.1002/(SICI)1097-0215(19961127)68:5<622::AID-IJC12>3.0.CO;2-3
PMID:8938145
Abstract

The amino acid sequence of the protein encoded by the gene MAGE-3 was screened for peptides containing the binding motif for HLA-B44. Nine peptides were synthesized, and their binding affinity for HLA-B4402 and -B4403 was analyzed in an HLA class I alpha-chain refolding assay. Four peptides with binding affinity for HLA-B4403 were chosen for in vitro cytotoxic T-lymphocyte induction assays using as antigen-presenting cells peptide-pulsed, autologous activated B lymphoblasts from a healthy, B4403+ donor. Peptide-specific effectors could be raised only against one peptide, M3-167. Cytotoxic T lymphocytes specific for this peptide were also able to recognize melanoma cell lines expressing HLA-B44 and the gene MAGE-3, strongly suggesting that M3-167 is a naturally processed MAGE-3-encoded epitope presented by HLA-B44. M3-167 is a I amino acid N-terminal extension of M3-168, a naturally processed epitope MAGE-3-encoded epitope presented by HLA-A1 that has been previously described. TAP binding studies of these 2 peptides revealed that the TAP affinity of M3-167 is about 9-fold higher than that of M3-168. M3-167 or a longer precursor could be transported into the endoplasmatic reticulum, where it could be trimmed for presentation by HLA-A1 or -B44 molecules. Taken together, our data suggest that M3-167 could be an immunodominant peptide encoded by the gene MAGE-3.

摘要

对由MAGE - 3基因编码的蛋白质的氨基酸序列进行筛选,寻找含有HLA - B44结合基序的肽段。合成了9种肽段,并在HLA I类α链重折叠试验中分析了它们与HLA - B4402和 - B4403的结合亲和力。选择了4种与HLA - B4403具有结合亲和力的肽段,用于体外细胞毒性T淋巴细胞诱导试验,使用来自健康的B4403 +供体的肽脉冲自体活化B淋巴母细胞作为抗原呈递细胞。仅对一种肽段M3 - 167能够产生肽特异性效应细胞。针对该肽段的细胞毒性T淋巴细胞也能够识别表达HLA - B44和MAGE - 3基因的黑色素瘤细胞系,强烈表明M3 - 167是由HLA - B44呈递的天然加工的MAGE - 3编码表位。M3 - 167是M3 - 168的I氨基酸N端延伸,M3 - 168是先前已描述的由HLA - A1呈递的天然加工的MAGE - 3编码表位。对这2种肽段的TAP结合研究表明,M3 - 167的TAP亲和力比M3 - 168高约9倍。M3 - 167或更长的前体可以转运到内质网中,在那里它可以被修剪以便由HLA - A1或 - B44分子呈递。综上所述,我们的数据表明M3 - 167可能是由MAGE - 3基因编码的免疫显性肽段。

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