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Pathogenic role of polyclonal and polymeric IgA in a murine model of mesangial proliferative glomerulonephritis with IgA deposition.

机译:多克隆和聚合型IgA在具有IgA沉积的系膜增生性肾小球肾炎的小鼠模型中的致病作用。

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摘要

Molecular size and charge distribution of IgA of sera and glomerular eluates were investigated in ddY mice, spontaneously developing mesangial proliferative glomerulonephritis (GN) with IgA deposition after 40 weeks of age. Serum IgA levels were increased in aged ddY mice more than 40 weeks old with a significant increase (P less than 0.01) at the age of 60 weeks, comparing with those of BALB/c mice. The isoelectric focusing (IEF) spectrotype of pooled serum IgA in 60-week-old mice ranged from 4.2 to 5.5, being similar to those in younger ddY (16 weeks old) and control BALB/c mice (12 weeks old) without enhanced expression of specific IgA peaks. However, IgA in the glomerular eluate from the 60-week-old mice showed limited anionic spectrotypes from pH 4.2 to 4.8. HPLC of IgA in pooled sera and glomerular eluates of 16-, 40- and 60-week-old ddY mice, revealed markedly increased ratios of the dimeric IgA (dIgA) and polymeric IgA (pIgA) in the total IgA with age. In the contrast to serum profiles, monomeric IgA (mIgA) was always detected as the smallest peak of the IgA fractions in glomerular eluates. Furthermore, aged mice with severe GN showed a higher percentage of dIgA and pIgA in total IgA (80%) in the sera than that of the mice with mild GN (64%). HPLC analysis under acid condition of glomerular IgA from 40-week-old ddY mice showed a similar pattern of dIgA and pIgA peaks in neutral buffer without the appearance of mIgA. These findings suggest that there is a selective mechanism for glomerular accumulation of more acid IgA among the polyclonally expanded IgA in old ddY mice, and that the polymeric form of IgA plays a pathogenic role in the development of mesangial proliferative GN in these mice.
机译:在ddY小鼠中研究了血清和肾小球洗脱液的IgA的分子大小和电荷分布,该小鼠在40周龄后自发发展了具有IgA沉积的肾小球系膜增生性肾小球肾炎(GN)。与BALB / c小鼠相比,超过40周龄的老龄ddY小鼠血清IgA水平升高,在60周龄时显着升高(P小于0.01)。 60周龄小鼠中合并的血清IgA的等电聚焦(IEF)谱图范围为4.2至5.5,与年轻的ddY(16周龄)和对照BALB / c小鼠(12周龄)相似,但表达没有增强IgA峰的数量。但是,来自60周龄小鼠的肾小球洗脱液中的IgA表现出有限的阴离子分型,pH值为4.2至4.8。 HPLC对16、40和60周龄ddY小鼠的血清和肾小球混合液中的IgA进行的HPLC分析显示,随着年龄的增长,二聚体IgA(dIgA)和聚合IgA(pIgA)的比例显着增加。与血清图相反,单体IgA(mIgA)始终被检测为肾小球洗脱液中IgA组分的最小峰。此外,患有严重GN的衰老小鼠血清中的dIgA和pIgA占总IgA的百分比(80%)比具有轻度GN的小鼠(64%)更高。在40周龄ddY小鼠的肾小球IgA酸性条件下进行的HPLC分析显示,在中性缓冲液中dIgA和pIgA峰的模式相似,而没有出现mIgA。这些发现表明,在老的ddY小鼠的多克隆扩展的IgA中,肾小球中更多的酸性IgA有选择性的积累机制,而IgA的聚合形式在这些小鼠的系膜增生性GN的发展中起着致病作用。

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