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来自感染疟疾的BALB/c小鼠的多克隆免疫球蛋白对(NZB×NZW)F1小鼠狼疮样综合征的有益作用。

Beneficial effect of polyclonal immunoglobulins from malaria-infected BALB/c mice on the lupus-like syndrome of (NZB x NZW)F1 mice.

作者信息

Hentati B, Sato M N, Payelle-Brogard B, Avrameas S, Ternynck T

机构信息

Départment d'Immunologie, CNRS URA 359, Institut Pasteur, Paris, France.

出版信息

Eur J Immunol. 1994 Jan;24(1):8-15. doi: 10.1002/eji.1830240103.

Abstract

We previously reported that infection of BALB/c mice with the parasite Plasmodium chabaudi induces high production of natural autoantibodies. Here we demonstrate that such an infection of lupus-prone (NZB x NZW)F1 (B/W) mice retards the development of their autoimmune disease. Survival and disease hallmarks (high-grade proteinuria and IgG anti-DNA antibodies) were delayed for 6 months when parasite inoculation was given at either 3 or 7 months of age, i.e. before or after the onset of the clinical symptoms. Similar beneficial effects, although less pronounced, were obtained when mice were treated with a total of 800 micrograms of IgG (P-IgG) or IgM (P-IgM) or 300 micrograms of cryoglobulin preparations isolated from P. chabaudi-infected BALB/c mice while similarly prepared fractions from uninfected mice had little effect. Compared to these fractions, P-IgG and P-IgM contained higher levels of natural antibodies bearing the D23 idiotype characteristic of polyreactive natural autoantibodies with enhanced activity against Fab and Fc fragments of IgG. In surviving mice, the level of anti-DNA antibodies, particularly those of IgG1 isotype, were significantly decreased. Flow cytometric analysis of various T cell subsets showed that the number of cells expressing gamma delta T cell receptor (TcR) antigens which did not vary with age was not modified after P-IgG or P-IgM treatment. In contrast, the number of T cells expressing V beta 8.1,2,V beta 10 and V beta 14 TcR antigens, which increased with age, were significantly reduced. Taken together, these results indicate that parasite infection of mice induces the synthesis of populations of IgM and IgG natural autoantibodies with immunoregulatory properties and that these antibodies attempt, at least transitorily, to rescue a natural autoantibody network that is deficient in B/W mice.

摘要

我们之前报道过,用查巴迪疟原虫感染BALB/c小鼠会诱导天然自身抗体的大量产生。在此我们证明,对易患狼疮的(NZB×NZW)F1(B/W)小鼠进行这样的感染会延缓其自身免疫疾病的发展。当在3个月或7个月龄时,即临床症状出现之前或之后进行寄生虫接种时,生存时间和疾病特征(重度蛋白尿和IgG抗DNA抗体)会延迟6个月。当用总共800微克的IgG(P-IgG)或IgM(P-IgM)或从感染查巴迪疟原虫的BALB/c小鼠中分离出的300微克冷球蛋白制剂处理小鼠时,也能获得类似的有益效果,尽管效果不太明显,而从未感染小鼠中制备的类似组分几乎没有效果。与这些组分相比,P-IgG和P-IgM含有更高水平的带有D23独特型的天然抗体,这种独特型是具有多反应性的天然自身抗体的特征,对IgG的Fab和Fc片段具有增强的活性。在存活的小鼠中,抗DNA抗体的水平,特别是IgG1同种型的抗体水平显著降低。对各种T细胞亚群的流式细胞术分析表明,表达γδT细胞受体(TcR)抗原的细胞数量不随年龄变化,在P-IgG或P-IgM处理后也没有改变。相比之下,表达Vβ8.1、2、Vβ10和Vβ14 TcR抗原的T细胞数量随年龄增加,在处理后显著减少。综上所述,这些结果表明,小鼠的寄生虫感染诱导了具有免疫调节特性的IgM和IgG天然自身抗体群体的合成,并且这些抗体至少在暂时范围内试图挽救B/W小鼠中缺陷的天然自身抗体网络。

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