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可溶性寄生虫产物可抑制实验性自身免疫性脑脊髓炎小鼠的临床症状,并差异调节人树突状细胞的活化。

Soluble helminth products suppress clinical signs in murine experimental autoimmune encephalomyelitis and differentially modulate human dendritic cell activation.

机构信息

Department of Molecular Cell Biology and Immunology, VU University Medical Center, Amsterdam, The Netherlands.

出版信息

Mol Immunol. 2012 Jun;51(2):210-8. doi: 10.1016/j.molimm.2012.03.020. Epub 2012 Apr 5.

DOI:10.1016/j.molimm.2012.03.020
PMID:22482518
Abstract

The increased incidence of auto-inflammatory and autoimmune diseases in the developed countries seems to be caused by an imbalance of the immune system due to the lack of proper regulation. Helminth parasites are well known modulators of the immune system and as such are of great interest for the treatment of these disorders. Clinical studies showed that administration of eggs of the pig nematode Trichuris suis to patients with inflammatory bowel disease reduces the disease severity. Here we demonstrate that treatment with soluble products from the nematodes T. suis and Trichinella spiralis induces significant suppression of symptoms in murine experimental autoimmune encephalomyelitis, a validated animal model for multiple sclerosis. These data show that infection with live nematodes is not a prerequisite for suppression of inflammation. To translate these results to the human system, the effects of soluble products of T. suis, T. spiralis and Schistosoma mansoni on the phenotype and function of human dendritic cells (DCs) were compared. Our data show that soluble products of T. suis, S. mansoni and T. spiralis suppress TNF-α and IL-12 secretion by TLR-activated human DCs, and that T. suis and S. mansoni, but not T. spiralis, strongly enhance expression of OX40L. Furthermore, helminth-primed human DCs differentially suppress the development of Th1 and/or Th17 cells. In conclusion, our data demonstrate that soluble helminth products have strong immunomodulatory capacities, but might exert their effects through different mechanisms. The suppressed secretion of pro-inflammatory cytokines together with an upregulation of OX40L expression on human DCs might contribute to achieve this modulation.

摘要

在发达国家,自身免疫性和自身炎症性疾病的发病率增加,似乎是由于缺乏适当的调节而导致免疫系统失衡所致。寄生虫是众所周知的免疫系统调节剂,因此对于治疗这些疾病具有重要意义。临床研究表明,给炎症性肠病患者服用猪蛔虫卵可减轻疾病的严重程度。在这里,我们证明了猪蛔虫和旋毛虫的可溶性产物的治疗可显著抑制实验性自身免疫性脑脊髓炎(多发性硬化症的一种验证动物模型)小鼠的症状。这些数据表明,感染活线虫并不是抑制炎症的前提条件。为了将这些结果转化为人体系统,比较了猪蛔虫、旋毛虫和曼氏血吸虫的可溶性产物对人树突状细胞(DC)表型和功能的影响。我们的数据表明,猪蛔虫、曼氏血吸虫和旋毛虫的可溶性产物可抑制 TLR 激活的人 DC 中 TNF-α和 IL-12 的分泌,而猪蛔虫和曼氏血吸虫但不是旋毛虫可强烈增强 OX40L 的表达。此外,寄生虫致敏的人 DC 可差异抑制 Th1 和/或 Th17 细胞的发育。总之,我们的数据表明,可溶性寄生虫产物具有很强的免疫调节能力,但可能通过不同的机制发挥作用。人 DC 上促炎细胞因子分泌的抑制以及 OX40L 表达的上调可能有助于实现这种调节。

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