曼氏血吸虫分泌一种抗炎、免疫调节因子。

Journal of inflammation Pub Date : 1995-01-01
K Ramaswamy, B Salafsky, S Potluri, Y X He, J W Li, T Shibuya
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引用次数: 0

摘要

曼氏血吸虫通过小鼠皮肤的渗透和迁移与炎症反应的减少有关,特别是在中度感染后。先前对曼氏血吸虫抑制人皮肤炎症反应机制的研究表明,曼氏血吸虫的排泄/分泌(ES)产物含有诱导人角质形成细胞产生抗炎细胞因子IL-1ra的活性。本研究对曼氏血吸虫ES产物进行了表征,以鉴定其诱导IL-1ra的活性。我们证明这种抗炎活性与分子质量为16.8 kDa (Sm 16.8)的蛋白有关。耗竭研究证实sm16.8是ES产物中主要的IL-1ra诱导活性。mansoni血吸虫和Trichobilharzia ocellata(一种能引起人类皮肤急性炎症的鸟血吸虫)的ES产物中蛋白质的比较表明,sm16.8在T. ocellata的ES产物中不存在。有趣的是,T. ocellata血吸虫的ES产物是人角质形成细胞IL-1 α的有效诱导性因子,而s. mansoni血吸虫的ES产物诱导角质形成细胞分泌IL-1 α很少或根本没有。功能研究表明sm16.8在体外抑制抗原诱导的淋巴细胞增殖反应。在脾脏或腋窝淋巴结细胞培养中添加sm16.8可显著降低抗原诱导的IL-2分泌。这些研究表明,曼氏血吸虫精心设计了一种抗炎、免疫调节因子,可能有助于寄生虫逃避宿主皮肤的免疫反应。鉴于sm16.8诱导IL-ira和抑制淋巴细胞增殖的能力,该蛋白也可能作为炎症性皮肤疾病的治疗剂。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Secretion of an anti-inflammatory, immunomodulatory factor by Schistosomulae of Schistosoma mansoni.

Penetration and migration of schistosomulae of Schistosoma mansoni through the skin of mice is associated with reduced inflammatory responses especially after a moderate infection. Previous studies to identify the mechanisms by which schistosomulae of S. mansoni suppress inflammatory responses in human skin showed that the excretory/secretory (ES) products of schistosomulae of s. mansoni contain activities that induce production of the antiinflammatory cytokine IL-1ra from human keratinocytes. In the present study we have characterized the ES products of the schistosomulae of S. mansoni to identify the IL-1ra inducing activity. We demonstrate that this anti-inflammatory activity is associated with a protein of molecular mass 16.8 kDa (Sm 16.8). Depletion studies confirm that Sm 16.8 is the major IL-1ra inducing activity in the ES products. A comparison of the proteins in the ES products of schistosomulae of S. mansoni with those of Trichobilharzia ocellata, a bird schistosome that induces an acute inflammation in human skin, shows that Sm 16.8 is absent in the ES products of T. ocellata. Interestingly, ES products of the schistosomulae of T. ocellata were potent inducers of IL-1 alpha from human keratinocytes, whereas ES products from schistosomulae of s. mansoni induce little or no IL-1 alpha secretion from keratinocytes. Functional studies show that Sm 16.8 suppresses antigen induced lymphoproliferative responses in vitro. Addition of Sm 16.8 to spleen or axillary lymph node cell cultures resulted in a significant reduction in antigen induced IL-2 secretion. These studies show that schistosomulae of S. mansoni elaborate an anti-inflammatory, immunomodulatory factor that may help the parasite to evade host immune responses in the skin. Given the capabilities of Sm 16.8 to induce IL-ira and suppress lymphoproliferation, this protein may also have a potential use as a therapeutic agent for inflammatory skin disorders.

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