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大疱性类天疱疮发病机制中的Th1、Th2和Th3细胞因子

Th1, Th2 and Th3 cytokines in the pathogenesis of bullous pemphigoid.

作者信息

Giomi Barbara, Caproni Marzia, Calzolari Anna, Bianchi Beatrice, Fabbri Paolo

机构信息

Department of Dermatological Science, University of Florence, Via degli Alfani 37, 50121 Florence, Italy.

出版信息

J Dermatol Sci. 2002 Nov;30(2):116-28. doi: 10.1016/s0923-1811(02)00067-1.

Abstract

Bullous pemphigoid (BP) is an autoimmune bullous skin disease mediated by autoantibodies against hemidesmosomal proteins. In addition to humoral immunity, the contribute of infiltrating T-helper (Th) autoreactive lymphocytes and their related cytokines to the pathomechanism of blistering is now growing in interest. To investigate T-cell activation markers and the presence of inflammatory and fibrogenic cytokines (i.e. IL2, IL-4, IL-5, IFN-gamma, TGF-beta) in BP lesional skin, we performed an immunohistochemical study and an in situ hybridization procedure on five BP patients, comparing them with two psoriatic patients and four healthy subjects. Our aim was to expand suitable information about tissutal expression of cytokines, secondly to further investigate the role of TGF-beta (a Th3-like or T-regulatory (T-reg) cytokine) in a non-scarring disorder like BP, in order to highlight its pleiotropic activity. The immunohistochemical analysis revealed a moderate to strong staining for IL-4 and IL-5 with a prevalent perivascular localization in the upper dermis. The staining for IFN-gamma showed a moderate/focal expression on the dermal perivascular infiltrate. IL-2 protein was observed in four cases. While no positive staining for IL-4 mRNA was detected in all BP subjects with in situ hybridization, IL-5 mRNA was documented in four BP specimens. A focal nuclear staining for IFN-gamma was observed in the epidermal layers and on the cellular infiltrate of lesional skin. In all BP cases, a moderate/diffuse positivity for TGF-beta(1) mRNA was documented in both cytoplasm and nucleus of the infiltrating perivascular cells of lesional and perilesional skin. Our results suggest a balance between Th1, Th2 and Th3 activity, with quantitatively different impact of the various cytokines on the pathomechanism of blistering, depending on the reciprocal network. The supposed participation of each cytokine analyzed in the pathogenesis of BP is discussed. The newest data obtained consist of TGF-beta detection in a non-scarring disease like PB, that had never been documented before, and in the confirmation of a mixed cytokine pattern in the fully developed phase of the disease.

摘要

大疱性类天疱疮(BP)是一种由针对半桥粒蛋白的自身抗体介导的自身免疫性大疱性皮肤病。除体液免疫外,浸润性辅助性T(Th)自身反应性淋巴细胞及其相关细胞因子在水疱形成病理机制中的作用目前越来越受到关注。为了研究BP皮损皮肤中T细胞活化标志物以及炎症和纤维化细胞因子(即白细胞介素2、白细胞介素4、白细胞介素5、γ干扰素、转化生长因子β)的存在情况,我们对5例BP患者进行了免疫组织化学研究和原位杂交检测,并将其与2例银屑病患者和4名健康受试者进行比较。我们的目的一是扩充有关细胞因子组织表达的合适信息,二是进一步研究转化生长因子β(一种Th3样或调节性T(T-reg)细胞因子)在像BP这样的非瘢痕性疾病中的作用,以突出其多效性活性。免疫组织化学分析显示白细胞介素4和白细胞介素5呈中度至强染色,在上层真皮中主要呈血管周围定位。γ干扰素染色在真皮血管周围浸润处呈中度/局灶性表达。在4例中观察到白细胞介素2蛋白。虽然原位杂交在所有BP受试者中均未检测到白细胞介素4 mRNA的阳性染色,但在4份BP标本中记录到白细胞介素5 mRNA。在表皮层和皮损皮肤的细胞浸润处观察到γ干扰素的局灶性核染色。在所有BP病例中,在皮损和皮损周围皮肤的血管周围浸润细胞的细胞质和细胞核中均记录到转化生长因子β(1) mRNA的中度/弥漫性阳性。我们的结果表明Th1、Th2和Th3活性之间存在平衡,各种细胞因子对水疱形成病理机制的影响在数量上有所不同,这取决于相互作用网络。讨论了所分析的每种细胞因子在BP发病机制中的假定参与情况。获得的最新数据包括在像PB这样的非瘢痕性疾病中检测到转化生长因子β,这在以前从未有过记录,以及在疾病的充分发展阶段证实了混合细胞因子模式。

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