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血清肾小球结合活性与MRL/lpr小鼠的肾脏疾病高度相关。

Serum glomerular binding activity is highly correlated with renal disease in MRL/lpr mice.

作者信息

Bernstein K A, Bolshoun D, Lefkowith J B

机构信息

Department of Medicine, Washington University School of Medicine, St Louis, MO 63110.

出版信息

Clin Exp Immunol. 1993 Sep;93(3):418-23. doi: 10.1111/j.1365-2249.1993.tb08194.x.

Abstract

The pathogenesis of lupus nephritis is felt to be mediated by anti-DNA antibodies. However, the anti-DNA response and renal disease do not entirely correspond. We recently developed a new assay which detects immune elements based on their ability to bind glomeruli as an alternative approach to understanding the pathogenesis of this disorder. The glomerular binding activity (GBA) defined by this assay consists of immune elements containing IgG which interact specifically with renal tissue, the binding of which is DNase-inhibitable, but which do not bind to DNA directly. In the current study we assessed the relationship between GBA and renal disease in MRL/lpr mice (both untreated and cyclophosphamide-treated) and compared it with the anti-DNA assay. Both assays were highly correlated with renal disease in untreated mice in terms of proteinuria. In cyclophosphamide-treated mice, however, only a weak correlation between the anti-DNA assay and proteinuria was apparent. GBA, in contrast, was more strongly correlated with proteinuria in treated mice. This correlation improved substantially when the DNase-sensitive component of the GBA was used. GBA appeared related to, but not covariant with, the anti-DNA response. These results demonstrate that GBA is a better correlate of murine lupus nephritis than the anti-DNA assay, and suggest that the immune elements detected by this assay, the DNase-sensitive component in particular, may be pathogenically important.

摘要

狼疮性肾炎的发病机制被认为是由抗DNA抗体介导的。然而,抗DNA反应与肾脏疾病并不完全对应。我们最近开发了一种新的检测方法,该方法基于免疫成分与肾小球结合的能力来检测免疫成分,以此作为理解这种疾病发病机制的另一种方法。通过该检测方法定义的肾小球结合活性(GBA)由含有IgG的免疫成分组成,这些免疫成分与肾组织特异性相互作用,其结合可被DNA酶抑制,但不直接与DNA结合。在当前研究中,我们评估了MRL/lpr小鼠(未治疗和环磷酰胺治疗)中GBA与肾脏疾病之间的关系,并将其与抗DNA检测进行比较。就蛋白尿而言,两种检测方法在未治疗小鼠中均与肾脏疾病高度相关。然而,在环磷酰胺治疗的小鼠中,抗DNA检测与蛋白尿之间仅呈现出微弱的相关性。相比之下,GBA与治疗小鼠中的蛋白尿相关性更强。当使用GBA中对DNA酶敏感的成分时,这种相关性显著改善。GBA似乎与抗DNA反应相关,但并非共变。这些结果表明,与抗DNA检测相比,GBA与小鼠狼疮性肾炎的相关性更好,并表明通过该检测方法检测到的免疫成分,特别是对DNA酶敏感的成分,可能在发病机制上具有重要意义。

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