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Suppression of type 2 immunity and allergic airway inflammation by secreted products of the helminth Heligmosomoides polygyrus

机译:抑制2型免疫和呼吸道过敏炎症分泌产物的寄生虫

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摘要

Allergic asthma is less prevalent in countries with parasitic helminth infections, and mice infected with parasites such as Heligmosomoides polygyrus are protected from allergic airway inflammation. To establish whether suppression of allergy could be mediated by soluble products of this helminth, we tested H. polygyrus excretory-secretory (HES) material for its ability to impair allergic inflammation. When HES was added to sensitising doses of ovalbumin, the subsequent allergic airway response was suppressed, with ablated cell infiltration, a lower ratio of effector (CD4 +CD25 +Foxp3 -) to regulatory (CD4 +Foxp3 +) T (Treg) cells, and reduced Th1, Th2 and Th17 cytokine production. HES exposure reduced IL-5 responses and eosinophilia, abolished IgE production and inhibited the type 2 innate molecules arginase-1 and RELM-α (resistin-like molecule-α). Although HES contains a TGF-β-like activity, similar effects in modulating allergy were not observed when administering mammalian TGF-β alone. HES also protected previously sensitised mice, suppressing recruitment of eosinophils to the airways when given at challenge, but no change in Th or Treg cell populations was apparent. Because heat-treatment of HES did not impair suppression at sensitisation, but compromised its ability to suppress at challenge, we propose that HES contains distinct heat-stable and heat-labile immunomodulatory molecules, which modulate pro-allergic adaptive and innate cell populations.
机译:过敏性哮喘是不流行的国家寄生蠕虫感染,和老鼠Heligmosomoides等感染寄生虫从过敏性气道polygyrus受到保护炎症。过敏可能是由可溶性的产品这种寄生虫,我们测试了h . polygyrusexcretory-secretory(他)材料能力影响过敏性炎症。卵清蛋白的加入使感光剂吗随后的气道反应是过敏抑制,与熔化的细胞渗透比率越低的效应(CD4 + CD25 + Foxp3)监管(CD4 + Foxp3 +) T细胞(Treg)减少Th1、Th2和Th17细胞因子的生产。他接触IL-5反应和减少嗜酸性粒细胞,废除IgE生产抑制了arginase-1 2型的分子和RELM -α(resistin-like分子-α)。他包含了TGF -β——活动,类似没有发现调制过敏的影响当管理哺乳动物TGF -β。以前也保护敏感老鼠,抑制嗜酸性粒细胞的招聘航空公司给出的挑战时,却没有改变或Treg细胞数量是明显的。热处理的他并没有损害抑制敏化作用,但损害的能力抑制在挑战,我们建议他包含不同的热稳定和heat-labile免疫调节分子,调节pro-allergic适应性和先天的细胞人群。

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