首页> 美国卫生研究院文献>The Journal of Clinical Investigation >Immune function in severe active rheumatoid arthritis. A relationship between peripheral blood mononuclear cell proliferation to soluble antigens and synovial tissue immunohistologic characteristics.
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Immune function in severe active rheumatoid arthritis. A relationship between peripheral blood mononuclear cell proliferation to soluble antigens and synovial tissue immunohistologic characteristics.

机译:严重的活动性类风湿关节炎的免疫功能。外周血单核细胞增殖对可溶性抗原与滑膜组织免疫组织学特征的关系。

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摘要

The immunohistology of synovium from a tender, swollen knee and peripheral blood cellular immune function were correlated in 24 clinically similar patients with active, seropositive rheumatoid arthritis who were not taking cytotoxic or long-acting antirheumatic drugs. The patients were classified as anergic (n = 6) or nonanergic (n = 18) on the basis of peripheral blood mononuclear cell proliferative responses to a battery of soluble recall antigens. The peripheral blood mononuclear cells of anergic patients failed to respond significantly to any soluble recall antigen, whereas cells from nonanergic patients responded to at least one such antigen. Multiple pieces of synovial tissue were obtained from each patient at arthroscopy. To minimize intrajoint variability, all pieces were analyzed and averaged to determine a composite profile of abnormalities. Synovial specimens from all six anergic patients had "high intensity" lymphocytic infiltration (group A). In sharp contrast, synovial specimens from 15 of 18 nonanergic patients had "low intensity" lymphocytic infiltration (group B) (P = 0.002). Group A tissues typically showed higher intensity T cell and plasma cell infiltration, more synovial lining layer hyperplasia, more HLA-DR bearing cells, and a higher ratio of Leu 3A/Leu 2A T cells than did group B. Group B tissues had fewer infiltrating cells (most of which were OKM1 and HLA-DR bearing), more extensive fibrin deposition, and far fewer T and plasma cells. Although these data do not imply that synovium from different joints in an individual patient are immunohistologically identical, they do provide evidence that peripheral blood mononuclear cell immune function reflects immunopathologic events in the biopsied joint. Moreover, the data further support the view that clinically active rheumatoid arthritis is, like certain other chronic inflammatory conditions, a heterogeneous disorder with polar subgroups.
机译:在24例临床上相似的活跃,血清反应阳性的类风湿关节炎患者中,未服用细胞毒性或长效抗风湿药的滑膜,膝关节肿胀和外周血细胞免疫功能与滑膜的免疫组织学相关。根据外周血对一系列可溶性召回抗原的单核细胞增殖反应,将患者分为无反应性(n = 6)或无反应性(n = 18)。厌氧患者的外周血单核细胞对任何可溶性召回抗原均无明显反应,而非厌氧患者的细胞对至少一种此类抗原反应。在关节镜检查时从每位患者获得多个滑膜组织。为了最大程度地减少关节内变异性,对所有部件进行分析并取平均值,以确定异常的综合特征。来自所有六名厌氧患者的滑膜标本具有“高强度”淋巴细胞浸润(A组)。与之形成鲜明对比的是,来自18位非贫血患者中15位的滑膜标本具有“低强度”淋巴细胞浸润(B组)(P = 0.002)。与B组相比,A组组织通常表现出更高的T细胞和浆细胞浸润强度,滑膜衬层增生,更多的HLA-DR承载细胞以及Leu 3A / Leu 2A T细胞比例更高。B组组织浸润较少细胞(其中大多数是OKM1和HLA-DR轴承),更广泛的纤维蛋白沉积以及少得多的T细胞和浆细胞。尽管这些数据并不意味着单个患者不同关节的滑膜在免疫组织学上是相同的,但它们确实提供了证据,即外周血单核细胞免疫功能反映了活检关节中的免疫病理事件。此外,数据进一步支持了这样的观点,即临床活跃的类风湿性关节炎与某些其他慢性炎症一样,是具有极性亚组的异质性疾病。

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