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在棕色挪威大鼠的HgCl2诱导的抗肾小球基底膜病模型中,多克隆激活后影响肾小球蛋白渗漏的因素。

Factors affecting the glomerular protein leak after polyclonal activation in the HgCl2-induced model of anti-GBM disease in the brown Norway rat.

作者信息

Savige J A, Lockwood C M

机构信息

Clinical Immunology Unit, Royal Postgraduate Medical School, London, UK.

出版信息

Clin Exp Immunol. 1987 Dec;70(3):619-29.

Abstract

The administration of the polyclonal activator HgCl2 (1 mg/kg i.p.) to Brown Norway (BN) rats on days 0, 2, 4 and 7 resulted in the cyclical production of anti-glomerular basement membrane (GBM) antibodies, the first peak of which occurred at day 14 with a smaller peak at day 26. Glomerular anti-GBM antibody levels were also raised at day 14. Renal injury as measured by urinary loss of albumin and complement (C3) was also cyclical, being maximal on days 15 and 23-26. However, urinary protein excretion was significantly diminished on the days corresponding to the first peak of circulating antibody levels if peripheral monocyte counts were reduced by the repeated injection of anti-monocyte antiserum. Protein excretion was also reduced after the administration of anti-polymorphonuclear neutrophil (PMN) antiserum. Finally, glomerular protein excretion was independent of depletion of serum C3 levels to less than 10% of pooled normal sera by the repeated administration of Cobra Venom Factor (CVF) on days 9 and 11. These findings demonstrate that in the absence of progressive tissue injury in this model, glomerular protein excretion fluctuates according to circulating levels of anti-GBM antibody and that, despite being independent of complement, tissue injury may be increased in the presence of complement activation.

摘要

在第0、2、4和7天给棕色挪威(BN)大鼠腹腔注射多克隆激活剂氯化汞(1毫克/千克),导致抗肾小球基底膜(GBM)抗体呈周期性产生,其第一个峰值出现在第14天,第26天出现一个较小的峰值。在第14天,肾小球抗GBM抗体水平也升高。通过白蛋白和补体(C3)的尿排泄量衡量的肾损伤也是周期性的,在第15天和第23 - 26天达到最大。然而,如果通过反复注射抗单核细胞抗血清降低外周单核细胞计数,在与循环抗体水平第一个峰值对应的日子里,尿蛋白排泄量会显著减少。注射抗多形核中性粒细胞(PMN)抗血清后,蛋白排泄量也会降低。最后,通过在第9天和第11天反复注射眼镜蛇毒因子(CVF)使血清C3水平降至合并正常血清的10%以下,肾小球蛋白排泄不受影响。这些发现表明,在该模型中不存在进行性组织损伤的情况下,肾小球蛋白排泄根据抗GBM抗体的循环水平波动,并且尽管与补体无关,但在补体激活的情况下组织损伤可能会增加。

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