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利用重组变应原开发针对昆虫叮咬超敏反应的预防性免疫方法:一项试点研究。

Developing a preventive immunization approach against insect bite hypersensitivity using recombinant allergens: A pilot study.

作者信息

Jonsdottir Sigridur, Hamza Eman, Janda Jozef, Rhyner Claudio, Meinke Andreas, Marti Eliane, Svansson Vilhjalmur, Torsteinsdottir Sigurbjorg

机构信息

Institute for Experimental Pathology, Biomedical Center, University of Iceland, Keldur, Keldnavegur 3, 112 Reykjavik, Iceland.

Department of Clinical Research and Veterinary Public Health, Vetsuisse Faculty, University of Berne, Länggassstrasse 124, 3012 Berne, Switzerland.

出版信息

Vet Immunol Immunopathol. 2015 Jul 15;166(1-2):8-21. doi: 10.1016/j.vetimm.2015.05.002. Epub 2015 May 15.

Abstract

Insect bite hypersensitivity (IBH) is an allergic dermatitis of horses caused by bites of midges (Culicoides spp.). IgE-mediated reactions are often involved in the pathogenesis of this disease. IBH does not occur in Iceland due to the absence of Culicoides, but it occurs with a high frequency in Icelandic horses exported to mainland Europe, where Culicoides are present. We hypothesize that immunization with the Culicoides allergens before export could reduce the incidence of IBH in exported Icelandic horses. The aim of the present study was therefore to compare intradermal and intralymphatic vaccination using four purified recombinant allergens, in combination with a Th1 focusing adjuvant. Twelve horses were vaccinated three times with 10μg of each of the four recombinant Culicoides nubeculosus allergens. Six horses were injected intralymphatically, three with and three without IC31(®), and six were injected intradermally, in the presence or absence of IC31(®). Antibody responses were measured by immunoblots and ELISA, potential sensitization in a sulfidoleukotriene release test and an intradermal test, cytokine and FoxP3 expression with real time PCR following in vitro stimulation of PBMC. Immunization with the r-allergens induced a significant increase in levels of r-allergen-specific IgG1, IgG1/3, IgG4/7, IgG5 and IgG(T). Application of the r-allergens in IC31(®) adjuvant resulted in a significantly higher IgG1, IgG1/3, IgG4/7 allergen-specific response. Intralymphatic injection was slightly more efficient than intradermal injection, but the difference did not reach significance. Testing of the blocking activity of the sera from the horses immunized intralymphatically with IC31(®) showed that the generated IgG antibodies were able to partly block binding of serum IgE from an IBH-affected horse to these r-allergens. Furthermore, IgG antibodies bound to protein bands on blots of C. nubeculosus salivary gland extract. No allergen-specific IgE was induced and there was no indication of induction of IgE-mediated reactions, as horses neither responded to Culicoides extract stimulation in a sulfidoleukotriene release test, nor developed a relevant immediate hypersensitivity reaction to the recombinant allergens in skin test. IL-4 expression was significantly higher in horses vaccinated intralymphatically without IC31(®), as compared to horses intradermally vaccinated with IC31(®). Both routes gave higher IL-10 expression with IC31(®). Both intralymphatic and intradermal vaccination of horses with recombinant allergens in IC31(®) adjuvant induced an immune response without adverse effects and without IgE production. The horses were not sensitized and produced IgG that could inhibit allergen-specific IgE binding. We therefore conclude that both the injection routes and the IC31(®) adjuvant are strong candidates for further development of immunoprophylaxis and therapy in horses.

摘要

昆虫叮咬超敏反应(IBH)是一种由蠓(库蠓属)叮咬引起的马过敏性皮炎。IgE介导的反应通常参与该疾病的发病机制。由于冰岛没有库蠓,所以IBH在冰岛不会发生,但在出口到有库蠓的欧洲大陆的冰岛马中却频繁发生。我们推测,在出口前用库蠓过敏原进行免疫接种可以降低出口冰岛马中IBH的发病率。因此,本研究的目的是比较使用四种纯化的重组过敏原并结合一种Th1偏向佐剂进行皮内和淋巴管内接种疫苗的效果。12匹马用10μg的四种重组库蠓过敏原各接种三次。6匹马进行淋巴管内注射,其中3匹使用IC31(®),3匹不使用;另外6匹马进行皮内注射,同样分别在有或没有IC31(®)的情况下进行。通过免疫印迹和ELISA检测抗体反应,在硫代白三烯释放试验和皮内试验中检测潜在的致敏情况,在体外刺激外周血单核细胞(PBMC)后用实时PCR检测细胞因子和FoxP3表达。用重组过敏原免疫接种后,r - 过敏原特异性IgG1、IgG1/3、IgG4/7、IgG5和IgG(T)水平显著升高。在IC31(®)佐剂中应用重组过敏原导致IgG1、IgG1/3、IgG4/7过敏原特异性反应显著更高。淋巴管内注射比皮内注射稍有效,但差异不显著。对用IC31(®)进行淋巴管内免疫接种的马的血清阻断活性进行检测表明,产生的IgG抗体能够部分阻断受IBH影响的马的血清IgE与这些重组过敏原的结合。此外,IgG抗体与库蠓唾液腺提取物印迹上的蛋白条带结合。未诱导出过敏原特异性IgE,也没有迹象表明诱导了IgE介导的反应,因为马在硫代白三烯释放试验中对库蠓提取物刺激无反应,在皮肤试验中对重组过敏原也未产生相关的速发型超敏反应。与用IC31(®)进行皮内接种的马相比,未使用IC31(®)进行淋巴管内接种的马中IL - 4表达显著更高。两种途径在使用IC31(®)时IL - 10表达均更高。用IC31(®)佐剂中的重组过敏原对马进行淋巴管内和皮内接种均诱导了免疫反应,且无不良反应,也未产生IgE。这些马未被致敏,并产生了能够抑制过敏原特异性IgE结合的IgG。因此,我们得出结论,注射途径和IC31(®)佐剂都是马免疫预防和治疗进一步发展的有力候选者。

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