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Expression of autoimmune regulator gene (AIRE) and T regulatory cells in human thymomas

机译:自身免疫调节基因(AIRE)和T调节细胞在人胸腺瘤中的表达

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摘要

Expression of the autoimmune regulator gene (AIRE) and the presence of CD25+/forkhead box p3 (FoxP3)+ T regulatory (Treg) cells were investigated in histologically normal adult thymi and in thymomas using immunohistochemistry and quantitative real-time polymerase chain reaction (PCR). In the normal thymus staining for AIRE was detected in the nucleus of some epithelial-like cells located in the medulla; in thymomas AIRE-positive cells were extremely rare and could be detected only in the areas of medullary differentiation of two B1 type, organoid thymomas. RNA was extracted from 36 cases of thymoma and 21 non-neoplastic thymi obtained from 11 myasthenic (MG+) and 10 non-myasthenic (MG) patients. It was found that AIRE is 8.5-fold more expressed in non-neoplastic thymi than in thymomas (P = 0.01), and that the amount of AIRE transcripts present in the thymoma tissue are not influenced by the association with MG, nor by the histological type. A possible involvement of AIRE in the development of MG was suggested by the observation that medullary thymic epithelial cells isolated from AIRE-deficient mice contain low levels of RNA transcripts for CHRNA 1, a gene coding for acetylcholine receptor. Expression of human CHRNA 1 RNA was investigated in 34 human thymomas obtained from 20 MG patients and 14 MG+ patients. No significant difference was found in the two groups (thymoma MG+, CHRNA1 = 0.013 ± 0.03; thymoma MG-, CHRNA1 = 0.01 ± 0.03). In normal and hyperplastic thymi CD25+/Foxp3+ cells were located mainly in the medulla, and their number was not influenced by the presence of MG. Foxp3+ and CD25+ cells were significantly less numerous in thymomas. A quantitative estimate of Treg cells revealed that the levels of Foxp3 RNA detected in non-neoplastic thymi were significantly higher (P = 0.02) than those observed in 31 cases of thymomas. Our findings indicate that the tissue microenvironment of thymomas is defective in the expression of relevant functions that exert a crucial role in the negative selection of autoreactive lymphocytes.
机译:在组织学正常的成年胸腺中研究了自身免疫调节基因(AIRE)的表达和CD25 + /叉头盒p3(FoxP3) + T调节(Treg)细胞的存在并在胸腺瘤中使用免疫组织化学和定量实时聚合酶链反应(PCR)。在正常的胸腺中,在位于延髓的一些上皮样细胞的细胞核中检测到了AIRE。在胸腺瘤中,AIRE阳性细胞极为稀少,仅在两种B1型器官样胸腺瘤的髓样分化区域才能检测到。从11例肌无力(MG + )和10例非肌无力(MG )患者中获得的36例胸腺瘤和21例非肿瘤性胸腺中提取RNA。发现非肿瘤性胸腺中AIRE的表达量比胸腺瘤中高8.5倍(P = 0.01),并且胸腺瘤组织中存在的AIRE转录本的量不受与MG的结合或组织学的影响类型。通过观察发现,从AIRE缺陷型小鼠分离的髓样胸腺上皮细胞含有低水平的CHRNA 1 RNA转录物,CHRNA 1是编码乙酰胆碱受体的基因,这表明AIRE可能参与了MG的发展。研究了从20名MG 患者和14名MG + 患者中获得的34例人胸腺瘤中人CHRNA 1 RNA的表达。两组均未发现显着差异(胸腺瘤MG + ,CHRNA1 = 0.013±0.03;胸腺瘤MG-,CHRNA1 = 0.01±0.03)。在正常和增生性胸腺CD25 + / Foxp3 + 细胞中,髓细胞主要位于髓质中,其数量不受MG的影响。在胸腺瘤中,Foxp3 + 和CD25 + 细胞的数量明显减少。 Treg细胞的定量估计显示,在非肿瘤性胸腺中检测到的Foxp3 RNA水平显着高于在31例胸腺瘤中观察到的水平(P = 0.02)。我们的发现表明,胸腺瘤的组织微环境在相关功能的表达方面存在缺陷,而相关功能在负反应性自身反应性淋巴细胞的选择中起着至关重要的作用。

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