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肿瘤相关分化抗原、MUC1糖型和癌胚抗原在人胸腺上皮细胞中的表达:对自身耐受性和肿瘤治疗的意义。

Expression of tumor-associated differentiation antigens, MUC1 glycoforms and CEA, in human thymic epithelial cells: implications for self-tolerance and tumor therapy.

作者信息

Cloosen Silvie, Arnold Janna, Thio Marco, Bos Gerard M J, Kyewski Bruno, Germeraad Wilfred T V

机构信息

Division of Hematology, Department of Internal Medicine, Growth and Development Research Institute, University Hospital Maastricht, the Netherlands.

出版信息

Cancer Res. 2007 Apr 15;67(8):3919-26. doi: 10.1158/0008-5472.CAN-06-2112.

DOI:10.1158/0008-5472.CAN-06-2112
PMID:17440107
Abstract

Expression of tissue-restricted self-antigens in the thymus, termed promiscuous gene expression, imposes T cell tolerance and protects from autoimmune diseases. This antigen pool also includes various types of tumor-associated antigens (TAA) previously thought to be secluded from the immune system. The scope of promiscuous gene expression has been defined by mRNA analysis at the global level of isolated medullary thymic epithelial cells (mTECs). Information at the protein level on the frequency of mTECs expressing a given antigen, on coexpression patterns, and post-translational modifications is largely missing. We report here promiscuous expression at the protein level of two TAA, MUC1 and CEA, in situ and in purified human mTECs. Both antigens are expressed in 1% to 3% of mTECs, either individually or coexpressed in the same cell. Using a panel of anti-MUC1 monoclonal antibodies recognizing different post-translational modifications, i.e., glycoforms of MUC1, we show that only fully glycosylated forms of MUC1 and the differentiation-dependent glycoforms were detected on mTECs, but not the cancer-associated glycoforms. Our findings imply that MUC1 and CEA are amenable to central tolerance induction, which might, however, be incomplete in case of tumor cell-restricted MUC1 glycoforms. Knowledge of these subtleties in promiscuous gene expression may, in the future, assist the selection of T cell tumor vaccines for clinical trials.

摘要

组织限制性自身抗原在胸腺中的表达,即所谓的混杂基因表达,可诱导T细胞耐受并预防自身免疫性疾病。这个抗原库还包括各种以前被认为与免疫系统隔绝的肿瘤相关抗原(TAA)。混杂基因表达的范围已通过对分离的胸腺髓质上皮细胞(mTEC)进行全局水平的mRNA分析来确定。关于表达特定抗原的mTEC频率、共表达模式和翻译后修饰的蛋白质水平信息在很大程度上还缺失。我们在此报告了两种TAA,即MUC1和CEA在原位和纯化的人mTEC中的蛋白质水平的混杂表达。这两种抗原在1%至3%的mTEC中表达,要么单独表达,要么在同一细胞中共表达。使用一组识别不同翻译后修饰(即MUC1糖型)的抗MUC1单克隆抗体,我们发现在mTEC上仅检测到完全糖基化形式的MUC1和分化依赖性糖型,而未检测到癌症相关糖型。我们的研究结果表明,MUC1和CEA易于诱导中枢耐受,然而,在肿瘤细胞限制性MUC1糖型的情况下,这种耐受可能并不完全。了解混杂基因表达中的这些细微差别,未来可能有助于选择用于临床试验的T细胞肿瘤疫苗。

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