小鼠抗原性关节炎中细胞粘附分子和细胞因子的表达。

G H Hersmann, J Kriegsmann, J Simon, C Hüttich, R Bräuer
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引用次数: 34

摘要

粘附分子和细胞因子在慢性炎症如类风湿关节炎(RA)中发挥着重要作用,它们在细胞活化和迁移中起着重要作用。应用免疫组织化学技术研究了抗原性关节炎动物模型小鼠膝关节冷冻切片中粘附分子和细胞因子的表达。各种粘附分子和细胞因子在关节炎关节组织中表达。LFA-1、Mac-1、CD44、ICAM-1和p -选择素在关节炎急性期强烈表达,在慢性期表达程度较低。vca -1和VCAM-1在第1天出现中等表达,l -选择素在第1 ~ 3天出现。LFA-1、Mac-1、CD44、α - 4整合素、ICAM-1和选择素在滑膜浸润细胞上表达,LFA-1、Mac-1和ICAM-1在滑膜衬里层表达,VCAM-1和p -选择素在内皮细胞上表达。在整个实验过程中,e -选择素在急性细胞浸润的细胞中低水平表达。细胞因子,尤其是IL-2、IL-4、IL-6、TNF和ifn - γ在关节炎急性期的细胞浸润中大量表达。综上所述,这些数据表明,细胞因子及其对粘附分子的激活有助于关节炎初始阶段的细胞浸润和激活,以及关节炎关节组织破坏的诱导和进展。这些分子可能是炎症和关节炎疾病新治疗策略的潜在靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Expression of cell adhesion molecules and cytokines in murine antigen-induced arthritis.

Adhesion molecules and cytokines are important in chronic inflammatory conditions such as rheumatoid arthritis (RA) by virtue of their role in cell activation and emigration. Using immunohistochemical techniques we studied the expression of adhesion molecules and cytokines in cryopreserved sections of murine knee joint in the course of antigen-induced arthritis, an animal model of human RA. Various adhesion molecules and cytokines are expressed in the arthritic joint tissue. LFA-1, Mac-1, CD44, ICAM-1 and P-selectin were strongly expressed in the acute phase and to a lesser degree in the chronic phase of arthritis. VLA-4 and VCAM-1 appeared to be moderately expressed on day 1, L-selectin between days 1 and 3. LFA-1, Mac-1, CD44, alpha 4-integrin, ICAM-1 and the selectins were found expressed on cells of the synovial infiltrate, LFA-1, Mac-1 and ICAM-1 on the synovial lining layer, and VCAM-1 and P-selectin on endothelial cells. Expression of E-selectin could be demonstrated throughout the experiment at a low level in cells of the acute cell infiltrate. Cytokines, especially IL-2, IL-4, IL-6, TNF, and IFN-gamma, were heavily expressed during the acute phase of arthritis in cellular infiltrate. Taken together these data demonstrate that cytokines and their activation of adhesion molecules contribute to cell infiltration and activation during the initial phase of arthritis and to the induction and progression of tissue destruction in arthritic joints. These molecules might be potential targets for novel therapeutic strategies in inflammatory and arthritic disorders.

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