首页> 美国卫生研究院文献>Annals of the Rheumatic Diseases >IgG3 cryoglobulins in autoimmune MRL-lpr/lpr mice: immunopathogenesis therapeutic approaches and relevance to similar human diseases.
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IgG3 cryoglobulins in autoimmune MRL-lpr/lpr mice: immunopathogenesis therapeutic approaches and relevance to similar human diseases.

机译:自身免疫性MRL-1pr / lpr小鼠中的IgG3冷冻球蛋白:免疫发病机制治疗方法和与类似人类疾病的相关性。

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摘要

MRL-lpr/lpr mice spontaneously develop an autoimmune disease resembling systemic lupus erythematosus and rheumatoid arthritis. One of the unique serological abnormalities in this strain is remarkably high concentrations of cryoglobulins. Analysis of immunoglobulin components in their cryoglobulins has shown selective enrichment of a particular IgG subclass, IgG3. As IgG3 enrichment is also found in two other cryoglobulins, which are induced after injection with bacterial lipopolysaccharides or infection with malaria, IgG3 apparently represents a major source of murine cryoglobulins. Studies on murine IgG3 monoclonal antibodies (mAbs) have clearly shown that murine IgG3 have the unique physiochemical property to self associate through non-specific IgG3 Fc-Fc interaction, and that most of them can generate monoclonal cryoglobulins. Most strikingly, IgG3 monoclonal cryoglobulins with rheumatoid factor (RF) activity induce extensive pathological manifestations: skin vascular purpura and glomerulonephritis with 'wire loop' lesions. Although the cryoglobulin activity of IgG3 RF mAb is solely responsible for the generation of glomerular lesions (both RF and cryoglobulin activities are necessary for skin vascular lesions), the absence of nephritogenic activity by some IgG3 cryoglobulins supports the idea that qualitative features of cryoglobulins are critical to determine their pathogenic activity. The demonstration of a positive correlation between the production of IgG3 cryoglobulins and the development of lupus nephritis in MRL-lpr/lpr mice further substantiates the pathological importance of cryogenic autoantibodies. On the other hand, it should be emphasised that non-cryogenerating IgG3 autoantibodies may not be harmful, but even protective, as a result of their interaction with pathogenic IgG3 cryoglobulins. Finally, the development of an experimental model of cryoglobulinaemia associated with vascular and glomerular disease certainly represents an invaluable opportunity to study the molecular mechanisms responsible for the generation of cryoglobulins and their associated tissue lesions, and also to assess various therapeutic approaches. Our demonstration that anti-idiotypic mAb can prevent the pathogenic effects of the cryoprecipitable IgG3 RF mAb suggests strongly that such a therapeutic approach might be successful in similar diseases in man.
机译:MRL-1pr / lpr小鼠自发发展为自身免疫性疾病,类似于系统性红斑狼疮和类风湿关节炎。该菌株独特的血清学异常之一是显着高浓度的冷球蛋白。对他们的冷球蛋白中免疫球蛋白成分的分析表明,特定的IgG亚类IgG3有选择性的富集。由于在注射细菌性脂多糖或感染疟疾后诱导的另外两种冷冻球蛋白中也发现了IgG3富集,因此IgG3显然是鼠类冷冻球蛋白的主要来源。对鼠IgG3单克隆抗体(mAb)的研究清楚地表明,鼠IgG3具有通过非特异性IgG3 Fc-Fc相互作用自缔合的独特理化特性,并且它们中的大多数可产生单克隆冷球蛋白。最引人注目的是,具有类风湿因子(RF)活性的IgG3单克隆球蛋白引起广泛的病理表现:皮肤血管性紫癜和肾小球肾炎伴“线loop”病变。尽管IgG3 RF mAb的冷冻球蛋白活性完全负责肾小球病变的产生(RF和冷冻球蛋白的活性对于皮肤血管病变都是必需的),但某些IgG3冷冻球蛋白缺乏产肾活性也支持这样的观点,即冷冻球蛋白的定性特征至关重要确定其致病活性。在MRL-1pr / lpr小鼠中IgG3冷冻球蛋白的产生与狼疮肾炎之间呈正相关的证明进一步证实了低温自身抗体的病理重要性。另一方面,应该强调的是,非低温生成的IgG3自身抗体可能与病原性IgG3低温球蛋白相互作用,因此可能不是有害的,甚至是保护性的。最后,与血管和肾小球疾病相关的冰球蛋白血症实验模型的开发无疑代表了一个宝贵的机会,可以研究引起冰球蛋白及其相关组织损伤的分子机制,并评估各种治疗方法。我们的抗独特型mAb可以预防可冷沉淀的IgG3 RF mAb的致病作用的证明强烈表明,这种治疗方法可能在人类的类似疾病中成功。

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