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犬利什曼病中免疫球蛋白G亚类分布:解读陷阱的综述与分析

Immunoglobulin G subclass distribution in canine leishmaniosis: a review and analysis of pitfalls in interpretation.

作者信息

Day M J

机构信息

Division of Veterinary Pathology, Infection and Immunity, School of Clinical Veterinary Science, University of Bristol, Langford BS40 5DU, United Kingdom.

出版信息

Vet Parasitol. 2007 Jun 20;147(1-2):2-8. doi: 10.1016/j.vetpar.2007.03.037. Epub 2007 Apr 27.

DOI:10.1016/j.vetpar.2007.03.037
PMID:17467176
Abstract

Infection with Leishmania may have different outcomes in genetically distinct individuals and the course of infection is determined by the nature of the host innate and adaptive immune response. Thus in experimentally infected mice, and in naturally infected dogs or humans, the protective (self-healing or asymptomatic) phenotype is associated with the induction of Th1-regulated cell-mediated immunity. By contrast, a Th2-regulated humoral immune response is associated with severe symptomatic disease. In the murine model system there is strong correlation between clinicopathological phenotype and the nature of the antigen-specific humoral immune response. Symptomatic infection and Th2-regulation is associated with elevation in antigen-specific IgG1 and IgE, whereas asymptomatic infection with Th1-regulation is linked with IgG2a production. IgG subclass restriction is less clear in human disease with only some clinical forms being correlated to a specific serological profile. Although numerous studies have questioned whether infected dogs develop skewed IgG subclass usage, the results of these have been conflicting-suggesting bias towards IgG1 or IgG2 or neither subclass in different investigations. This confusion could relate to the specificity of the commercially available polyclonal antisera used to detect the canine IgG1 and IgG2 subclasses. More meaningful results might be obtained by the use of the panel of monoclonal antibodies with well-validated specificity for all four canine IgG subclasses.

摘要

利什曼原虫感染在基因不同的个体中可能有不同的结果,感染过程由宿主固有免疫和适应性免疫反应的性质决定。因此,在实验感染的小鼠以及自然感染的犬类或人类中,保护性(自愈或无症状)表型与Th1调节的细胞介导免疫的诱导相关。相比之下,Th2调节的体液免疫反应与严重的症状性疾病相关。在小鼠模型系统中,临床病理表型与抗原特异性体液免疫反应的性质之间存在很强的相关性。症状性感染和Th2调节与抗原特异性IgG1和IgE升高相关,而Th1调节的无症状感染与IgG2a产生相关。在人类疾病中,IgG亚类限制不太明显,只有一些临床形式与特定的血清学特征相关。尽管许多研究质疑感染犬是否会出现IgG亚类使用偏向,但这些研究结果相互矛盾,在不同调查中显示出对IgG1或IgG2的偏向或两者均无偏向。这种混淆可能与用于检测犬IgG1和IgG2亚类的市售多克隆抗血清的特异性有关。使用对所有四种犬IgG亚类具有充分验证特异性的单克隆抗体组合可能会获得更有意义的结果。

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