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硬化性苔藓的比较免疫表型研究:亲表皮性CD57 +淋巴细胞数量众多——对发病机制的启示

Comparative immunophenotypic study of lichen sclerosus: epidermotropic CD57+ lymphocytes are numerous--implications for pathogenesis.

作者信息

Carlson J A, Grabowski R, Chichester P, Paunovich E, Malfetano J

机构信息

Division of Dermatopathology, Albany Medical College, New York 12208, USA.

出版信息

Am J Dermatopathol. 2000 Feb;22(1):7-16. doi: 10.1097/00000372-200002000-00002.

Abstract

To characterize the immunophenotype of inflammatory cells in lichen sclerosus (LS), we performed a comparative case control study using one- and two-color immunohistochemistry and the nitro blue tetrazolium (NBT) reaction. Study material consisted of 100 biopsies from patients with LS or from 12 control groups consisting of inflammatory, scarring, and depigmenting cutaneous disorders. In addition, fresh tissue was sampled from four vulvectomy specimens for NBT testing. The typical inflammatory infiltrate of LS contained numerous epidermotropic CD3+, CD8+, CD57+ cells, increased intraepidermal HLA-DR+ cells, and a dermal infiltrate rich in CD8+, CD57+, HLA-DR+, and CD68+ inflammatory cells. Comparing LS to the 12 control groups, epidermotropic CD57+ lymphocytes independently predicted LS (P = 0.006, logistic regression, multivariate analysis). Among the 12 control groups, only specimens of the inflammatory stage of morphea exhibited numerous dermal CD57+ lymphocytes. Two-color immunohistochemistry confirmed the CD3+/CD8+CD57+ and CD3+/ CD8+/CD57+HLA-DR+ epidermotropic and dermal lymphocytic phenotypes and the dermal macrophage CD68+HLA-DR+ phenotype. In LS, the NBT reaction revealed evidence of superoxide production associated with CD68+HLA-DR+ cells. Expansion of CD8+CD57+lymphocytes is associated with viral infections, autoimmune disease, malignancies, and transplantation and is suspected to be the result of chronic excessive antigen challenge. In these pathologic states, CD8+CD57+ lymphocytes (as terminally differentiated, antigen-specific T cells) participate in the suppression of cytolytic activity to limit tissue damage. In LS, activated macrophages and lymphocytes indicate persistent antigen-driven inflammation. LS's numerous CD8+CD57+ lymphocytes may be either the mediators or the consequence of its hallmark sclerosis.

摘要

为了描述硬化性苔藓(LS)中炎症细胞的免疫表型,我们使用单克隆和双色免疫组织化学以及硝基蓝四氮唑(NBT)反应进行了一项比较病例对照研究。研究材料包括来自LS患者的100份活检样本,或来自12个对照组,这些对照组由炎症性、瘢痕性和色素脱失性皮肤疾病组成。此外,从4份外阴切除标本中采集新鲜组织进行NBT检测。LS典型的炎症浸润包含大量亲表皮的CD3⁺、CD8⁺、CD57⁺细胞,表皮内HLA-DR⁺细胞增多,以及真皮浸润富含CD8⁺、CD57⁺、HLA-DR⁺和CD68⁺炎症细胞。将LS与1十二对照组进行比较,亲表皮的CD57⁺淋巴细胞可独立预测LS(P = 0.006,逻辑回归,多变量分析)。在12个对照组中,只有硬斑病炎症期的标本显示出大量真皮CD57⁺淋巴细胞。双色免疫组织化学证实了亲表皮和真皮淋巴细胞的CD3⁺/CD8⁺CD57⁺以及CD3⁺/CD8⁺/CD57⁺HLA-DR⁺表型,以及真皮巨噬细胞的CD68⁺HLA-DR⁺表型。在LS中,NBT反应显示与CD68⁺HLA-DR⁺细胞相关的超氧化物产生证据。CD8⁺CD57⁺淋巴细胞的扩增与病毒感染、自身免疫性疾病、恶性肿瘤和移植有关,并且怀疑是慢性过度抗原刺激的结果。在这些病理状态下,CD8⁺CD57⁺淋巴细胞(作为终末分化的抗原特异性T细胞)参与细胞溶解活性的抑制以限制组织损伤。在LS中,活化的巨噬细胞和淋巴细胞表明存在持续的抗原驱动炎症。LS中大量的CD8⁺CD57⁺淋巴细胞可能是其标志性硬化的介质或结果。

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