类风湿关节炎患者滑膜类成纤维细胞在细胞接触诱导促炎细胞因子产生过程中依赖和不依赖VLA - 4的途径

VLA-4-dependent and -independent pathways in cell contact-induced proinflammatory cytokine production by synovial nurse-like cells from rheumatoid arthritis patients.

作者信息

Takeuchi Eiji, Tanaka Toshiyuki, Umemoto Eiji, Tomita Tetsuya, Shi Kenrin, Takahi Koichiro, Suzuki Ryuji, Ochi Takahiro, Miyasaka Masayuki

机构信息

Laboratory of Molecular and Cellular Recognition, Osaka University Graduate School of Medicine, Japan.

出版信息

Arthritis Res. 2002;4(6):R10. doi: 10.1186/ar593. Epub 2002 Aug 12.

DOI:10.1186/ar593

PMID:12453313

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC153839/

Abstract

Nurse-like stromal cell lines from the synovial tissue of patients with rheumatoid arthritis (RA-SNC) produce, on coculture with lymphocytes, large amounts of proinflammatory cytokines. In the present paper, we analyze the molecular events necessary for the induction of cytokine release from RA-SNC cells, and particularly the roles played by cell adhesion and the transmigration (also known as pseudoemperipolesis) of lymphocytes. For this purpose, the effects of various mAbs on the binding and transmigration of a human B-cell line, MC/car, were examined using a cloned RA-SNC line, RA-SNC77. To analyze the role of lymphocyte binding and transmigration on upregulated cytokine production by the RA-SNC77 cells, we used C3 exoenzyme-treated MC/car cells, which could bind to RA-SNC77 cells but could not transmigrate. Treatment with anti-CD29 or anti-CD49d mAb significantly reduced binding and transmigration of the MC/car cells. In contrast, the neutralizing anti-CD106/vascular cell adhesion molecule 1 mAb did not show any inhibitory effect. Likewise, none of the neutralizing mAbs against CD11a, CD18, CD44, CD49e, or CD54 showed significant effects. Binding of C3-treated or untreated MC/car cells to RA-SNC77 cells induced comparable levels of IL-6 and IL-8 production. In addition, the enhanced cytokine production by RA-SNC77 cells required direct lymphocyte contact via a very late antigen-4 (VLA-4)-independent adhesion pathway. These results indicate that, although both the VLA-4-dependent/vascular cell adhesion molecule 1-independent and the VLA4-independent adhesion pathways are involved in MC/car binding and subsequent transmigration, only the VLA4-independent adhesion pathway is necessary and sufficient for the enhanced proinflammatory cytokine production by RA-SNC77 cells. The transmigration process, which is dependent on Rho-GTPase, is not a prerequisite for this phenomenon.

摘要

来自类风湿性关节炎患者滑膜组织的类护士基质细胞系（RA - SNC）与淋巴细胞共培养时会产生大量促炎细胞因子。在本文中，我们分析了诱导RA - SNC细胞释放细胞因子所需的分子事件，特别是细胞黏附以及淋巴细胞迁移（也称为假包绕现象）所起的作用。为此，使用克隆的RA - SNC系RA - SNC77研究了各种单克隆抗体对人B细胞系MC/car的结合和迁移的影响。为了分析淋巴细胞结合和迁移对RA - SNC77细胞上调细胞因子产生的作用，我们使用了经C3外切酶处理的MC/car细胞，其可与RA - SNC77细胞结合但不能迁移。用抗CD29或抗CD49d单克隆抗体处理可显著降低MC/car细胞的结合和迁移。相反，中和性抗CD106/血管细胞黏附分子1单克隆抗体未显示任何抑制作用。同样，针对CD11a、CD18、CD44、CD49e或CD54的中和性单克隆抗体均未显示显著作用。C3处理或未处理的MC/car细胞与RA - SNC77细胞的结合诱导了相当水平的IL - 6和IL - 8产生。此外，RA - SNC77细胞增强的细胞因子产生需要通过一条不依赖极迟抗原 - 4（VLA - 4）的黏附途径进行直接的淋巴细胞接触。这些结果表明，虽然依赖VLA - 4/不依赖血管细胞黏附分子1的黏附途径以及不依赖VLA4的黏附途径均参与了MC/car的结合及随后的迁移，但只有不依赖VLA4的黏附途径对于RA - SNC77细胞增强促炎细胞因子的产生是必要且充分的。依赖Rho - GTP酶的迁移过程并非此现象的先决条件。