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重症肌无力:增生性和肿瘤性胸腺微环境组织中的免疫组织学异质性提示耐受性破坏的不同机制。

Myasthenia gravis: immunohistological heterogeneity in microenvironmental organization of hyperplastic and neoplastic thymuses suggesting different mechanisms of tolerance breakdown.

作者信息

Chilosi M, Iannucci A, Fiore-Donati L, Tridente G, Pampanin M, Pizzolo G, Ritter M, Bofill M, Janossy G

出版信息

J Neuroimmunol. 1986 May;11(3):191-204. doi: 10.1016/0165-5728(86)90003-2.

Abstract

Four samples of thymoma obtained from patients affected by myasthenia gravis have been immunohistologically analysed on cryostat sections using a panel of antisera and monoclonal antibodies specific for antigens which define different stages of intrathymic lymphocyte differentiation and antigens specific for different types of thymic epithelial cells (cortical, medullary). When the thymoma samples were compared to age-matched normal thymuses and hyperplastic thymuses obtained from patients with myasthenia gravis some evident microenvironmental differences could be demonstrated using these reagents. In all the thymoma samples in fact the neoplastic lobules appeared as grossly enlarged cortical-type areas, formed by accumulations of T lymphocytes exhibiting the cortical immature phenotype (TdT+, T6+, etc.) within a network of putatively neoplastic epithelial cells characterized by cortical phenotype as defined by reactivity with various monoclonal antibodies (RFD4-, MR3+). These 'cortical' epithelia showed some abnormal features such as lack or irregular distribution of HLA-DR and enhanced keratin expression. Small areas of 'medullary' differentiation could be observed in 3/4 thymoma samples. In thymic hyperplasia, on the other hand, the cortical areas appeared somewhat compressed (but comparable to those observed in normal age-matched samples) by enlarged medullary areas. The expansion of medullary areas was due to the infiltration of 'peripheral' lymphoid tissue intruding through the extraparenchymal zone and forming organized B and T areas. These observations are discussed in the light of the clinical heterogeneity observed in myasthenia gravis.

摘要

对4例重症肌无力患者的胸腺瘤样本进行了免疫组织学分析,采用一组抗血清和单克隆抗体,这些抗体针对定义胸腺内淋巴细胞分化不同阶段的抗原以及不同类型胸腺上皮细胞(皮质型、髓质型)的特异性抗原。当将胸腺瘤样本与年龄匹配的正常胸腺以及重症肌无力患者的增生性胸腺进行比较时,使用这些试剂可显示出一些明显的微环境差异。实际上,在所有胸腺瘤样本中,肿瘤小叶表现为明显增大的皮质型区域,由T淋巴细胞聚集形成,这些T淋巴细胞表现出皮质未成熟表型(TdT +、T6 +等),位于假定的肿瘤上皮细胞网络内,这些上皮细胞具有皮质表型,通过与各种单克隆抗体(RFD4 -、MR3 +)反应来定义。这些“皮质”上皮显示出一些异常特征,如HLA - DR缺乏或分布不规则以及角蛋白表达增强。在4个胸腺瘤样本中的3个中可观察到小面积的“髓质”分化。另一方面,在胸腺增生中,皮质区域似乎被扩大的髓质区域压缩(但与年龄匹配的正常样本中观察到的区域相当)。髓质区域的扩张是由于“外周”淋巴组织通过实质外区域浸润并形成有组织的B和T区域所致。根据重症肌无力中观察到的临床异质性对这些观察结果进行了讨论。

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