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通过抗细胞间粘附分子ICAM - 1抗体抑制实验性变应性神经炎

Suppression of experimental allergic neuritis by an antibody to the intracellular adhesion molecule ICAM-1.

作者信息

Archelos J J, Mäurer M, Jung S, Toyka K V, Hartung H P

机构信息

Department of Neurology, Julius-Maximilians-Universität Würzburg, Germany.

出版信息

Brain. 1993 Oct;116 ( Pt 5):1043-58. doi: 10.1093/brain/116.5.1043.

Abstract

Experimental allergic (autoimmune) neuritis (EAN) was induced in Lewis rats either by inoculation with bovine spinal root myelin or injection of neuritogenic P2-specific T cells. Injection of a purified monoclonal antibody (1A-29) to the intercellular adhesion molecule-1 (ICAM-1) prevented or transiently suppressed myelin-induced EAN depending on the timing of antibody application. Administration of 1A-29 suppressed moderate adoptive transfer EAN (AT-EAN) but not severe AT-EAN. In contrast, treatment with phosphate buffered saline or an unrelated IgG1 had no effect on the course of the disease. Histological sections of the peripheral nervous system (PNS) showed a marked reduction of inflammatory infiltrates and perivascular demyelination in rats injected with 1A-29. The effect of 1A-29 on the concanavalin A (Con A)- and P2-dependent proliferation of neuritogenic P2-specific T cells was studied in vitro. Our data suggest that antibodies to ICAM-1 act on the induction and effector phase of the immune response by inhibiting both early interactions between immunocompetent cells after exposure to foreign antigen and transendothelial migration of primed T cells into the peripheral nerve. Treatment with antibodies to leucocyte adhesion molecules could be a useful therapeutic approach to autoimmune disease of the PNS.

摘要

通过接种牛脊髓根髓磷脂或注射致神经炎的P2特异性T细胞,在Lewis大鼠中诱发实验性变应性(自身免疫性)神经炎(EAN)。注射针对细胞间黏附分子-1(ICAM-1)的纯化单克隆抗体(1A-29),根据抗体应用的时机,可预防或短暂抑制髓磷脂诱导的EAN。给予1A-29可抑制中度过继转移EAN(AT-EAN),但对重度AT-EAN无效。相比之下,用磷酸盐缓冲盐水或无关的IgG1进行治疗对疾病进程没有影响。外周神经系统(PNS)的组织学切片显示,注射1A-29的大鼠中炎性浸润和血管周围脱髓鞘明显减少。在体外研究了1A-29对刀豆蛋白A(Con A)和P2依赖性致神经炎P2特异性T细胞增殖的影响。我们的数据表明,抗ICAM-1抗体通过抑制接触外来抗原后免疫活性细胞之间的早期相互作用以及致敏T细胞跨内皮迁移至周围神经,作用于免疫反应的诱导期和效应期。用抗白细胞黏附分子抗体进行治疗可能是治疗PNS自身免疫性疾病的一种有用的治疗方法。

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