首页> 美国卫生研究院文献>The Journal of Clinical Investigation >An in vitro assay for detection of glomerular binding IgG autoantibodies in patients with systemic lupus erythematosus.
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An in vitro assay for detection of glomerular binding IgG autoantibodies in patients with systemic lupus erythematosus.

机译:用于检测系统性红斑狼疮患者肾小球结合IgG自身抗体的体外检测方法。

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摘要

The deposition of anti-dsDNA antibodies in the glomerulus is believed to play a critical role in the pathogenesis of nephritis in SLE. However, an absolute correlation between serum levels of anti-dsDNA antibodies and renal disease has not been found. Recently a glomerular binding assay (GBA) has been developed to detect IgG binding to isolated rat glomeruli. We have used the GBA to study sera from four groups of SLE patients: (A) + anti-dsDNA antibodies, active nephritis; (B) - anti-dsDNA antibodies, active nephritis; (C) + anti-dsDNA antibodies, no nephritis; and (D) - anti-dsDNA antibodies, no nephritis. The serum anti-dsDNA antibodies in group A and group C patients could not be distinguished on the basis of isotype, charge, or cross-reactivity with histones. Nevertheless, the mean intensity of glomerular immunofluorescence was significantly higher in group A than in the three other patient groups and distinguished between patients with serum anti-dsDNA antibodies who had nephritis and those without clinically apparent nephritis. GBA reactivity was unaffected by DNase treatment of sera, but was partially inhibited by preincubation with dsDNA. These findings are consistent with the hypothesis that some anti-dsDNA antibodies cross-react with glomerular components and that the presence of this cross-reactivity is associated with, and may be responsible for, the development of nephritis. In addition, we have identified a group of SLE patients with renal disease and typical renal histopathology and immune deposits who do not have serum anti-dsDNA antibodies or antibodies that directly bind to glomeruli in the GBA. The mechanism of renal immune deposition in these patients remains to be determined.
机译:据信抗dsDNA抗体在肾小球中的沉积在SLE中肾炎的发病机理中起关键作用。然而,尚未发现抗dsDNA抗体的血清水平与肾脏疾病之间的绝对相关性。最近,已经开发出一种肾小球结合测定法(GBA)来检测IgG与分离的大鼠肾小球的结合。我们已经使用GBA研究了四组SLE患者的血清:(A)+抗dsDNA抗体,活动性肾炎; (B)-抗dsDNA抗体,活动性肾炎; (C)+抗dsDNA抗体,无肾炎; (D)-抗dsDNA抗体,无肾炎。 A组和C组患者的血清抗dsDNA抗体无法根据组蛋白的同种型,电荷或交叉反应来区分。尽管如此,A组肾小球免疫荧光的平均强度显着高于其他三个患者组,并且在患有肾炎的血清抗dsDNA抗体患者和没有临床上明显的肾炎的患者之间进行了区分。 GBA反应性不受DNase处理血清的影响,但被dsDNA预温育部分抑制。这些发现与以下假设一致:一些抗dsDNA抗体与肾小球成分发生交叉反应,并且这种交叉反应的存在与肾炎的发生有关,并可能与之相关。此外,我们已经鉴定出一组患有肾脏疾病,典型的肾脏组织病理学和免疫沉积物的SLE患者,这些患者没有血清抗dsDNA抗体或与GBA中的肾小球直接结合的抗体。这些患者中肾脏免疫沉积的机制尚待确定。

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