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人白细胞抗原I类抗原加工机制在髓母细胞瘤中的表达及功能分析

Expression and functional analysis of human leukocyte antigen class I antigen-processing machinery in medulloblastoma.

作者信息

Raffaghello Lizzia, Nozza Paolo, Morandi Fabio, Camoriano Marta, Wang Xinhui, Garrè Maria Luisa, Cama Armando, Basso Giuseppe, Ferrone Soldano, Gambini Claudio, Pistoia Vito

机构信息

Laboratories of Oncology, G. Gaslini Institute, Genoa, Italy.

出版信息

Cancer Res. 2007 Jun 1;67(11):5471-8. doi: 10.1158/0008-5472.CAN-06-4735.

DOI:10.1158/0008-5472.CAN-06-4735
PMID:17545629
Abstract

Defects in the expression and/or function of the human leukocyte antigen (HLA) class I antigen-processing machinery (APM) components are found in many tumor types. These abnormalities may have a negative impact on the interactions of tumor cells with host's immune system and on the outcome of T cell-based immunotherapy. To the best of our knowledge, no information is available about APM component expression and functional characteristics in human medulloblastoma cells (Mb). Therefore, in the present study, we have initially compared the expression of APM components in Mb, an embryonal pediatric brain tumor with a poor prognosis, with that in noninfiltrating astrocytic pediatric tumors, a group of differentiated brain malignancies with favorable prognosis. LMP2, LMP7, calnexin, beta2-microglobulin-free heavy chain (HC) and beta2-microglobulin were down-regulated or undetectable in Mb lesions, but not in astrocytic tumors or normal fetal cerebellum. Two Mb cell lines (DAOI and D283) displayed similar but not superimposable defects in APM component expression as compared with primary tumors. To assess the functional implications of HLA class I APM component down-regulation in Mb cell lines, we tested their recognition by HLA class I antigen-restricted, tumor antigen (TA)-specific CTL, generated by stimulations with dendritic cells that had been transfected with Mb mRNA. The Mb cell lines were lysed by TA-specific CTL in a HLA-restricted manner. Thus, defective expression of HLA class I-related APM components in Mb cells does not impair their ability to present TA to TA-specific CTL. In conclusion, these results can contribute to optimize T cell-based immunotherapeutic strategies for Mb treatment.

摘要

在许多肿瘤类型中都发现了人类白细胞抗原(HLA)I类抗原加工机制(APM)成分的表达和/或功能缺陷。这些异常可能会对肿瘤细胞与宿主免疫系统的相互作用以及基于T细胞的免疫治疗结果产生负面影响。据我们所知,目前尚无关于人类髓母细胞瘤细胞(Mb)中APM成分表达和功能特征的信息。因此,在本研究中,我们首先比较了预后较差的胚胎性小儿脑肿瘤Mb与预后良好的非浸润性星形细胞小儿肿瘤(一组分化型脑恶性肿瘤)中APM成分的表达。LMP2、LMP7、钙连接蛋白、无β2-微球蛋白的重链(HC)和β2-微球蛋白在Mb病变中下调或无法检测到,但在星形细胞瘤或正常胎儿小脑中未出现这种情况。与原发性肿瘤相比,两种Mb细胞系(DAOI和D283)在APM成分表达上表现出相似但并非完全重叠的缺陷。为了评估Mb细胞系中HLA I类APM成分下调的功能影响,我们测试了它们被经Mb mRNA转染的树突状细胞刺激产生的HLA I类抗原限制性、肿瘤抗原(TA)特异性CTL识别的情况。Mb细胞系以HLA限制性方式被TA特异性CTL裂解。因此,Mb细胞中HLA I类相关APM成分的缺陷表达并不损害它们将TA呈递给TA特异性CTL的能力。总之,这些结果有助于优化基于T细胞的Mb免疫治疗策略。

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