首页> 外文期刊>The Journal of Experomental Medicine >Clonotypic heterogeneity in experimental interstitial nephritis. Restricted specificity of the anti-tubular basement membrane B cell repertoire is associated with a disease-modifying crossreactive idiotype.
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Clonotypic heterogeneity in experimental interstitial nephritis. Restricted specificity of the anti-tubular basement membrane B cell repertoire is associated with a disease-modifying crossreactive idiotype.

机译:实验性间质性肾炎的Clonotypic异质性。抗肾小管基底膜B细胞库的特异性受限与疾病缓解的交叉反应性独特型有关。

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Experimental anti-tubular basement membrane (anti-TBM) disease is an autoimmune interstitial nephritis elicited in susceptible rodents after immunization with renal tubular antigen. The nephritogenic antigen in the immunizing preparation is 3M-1, a 48,000 Mr noncollagenous glycoprotein. The hallmarks of the renal lesion are the presence of anti-TBM antibodies (anti-TBM-Ab) and a dense mononuclear cell infiltrate. The anti-TBM B cell repertoire in this disease was analyzed using a library of 22 anti-TBM mAbs generated in a prototypically susceptible Brown Norway rat. These anti-TBM mAbs were all demonstrated to be 3M-1 specific and their characterization formed the basis for the following observations: (a) The size of the anti-TBM B cell population is estimated at 58 distinct clones; (b) by competitive inhibition criteria, all anti-TBM mAbs recognize the same (or spatially close) epitope(s) on 3M-1. This focused recognition was maintained in spite of considerable variability in affinity. Epitopic dominance could also be demonstrated in human polyclonal anti-TBM antisera from a patient with anti-TBM disease; and (c) a crossreactive idiotype was documented, and antisera directed toward this set of variable region determinants was shown to be effective as a prophylactic regimen to abrogate disease, and as a therapeutic modality to arrest the progression of disease; (d) analysis of VH gene families suggested biased usage of Q52- and 7183-like families, although at least three gene families are used in the anti-TBM-Ab response. Thus, the anti-TBM B cell compartment in BN rats is moderately large, but is primarily focused to a single epitope on the nephritogenic antigen and is associated with a disease-modifying crossreactive idiotype.
机译:实验性抗肾小管基底膜(anti-TBM)疾病是用肾小管抗原免疫后在易感啮齿动物中引发的自身免疫性间质性肾炎。免疫制剂中产生肾炎的抗原是3M-1,一种48,000 Mr非胶原糖蛋白。肾病变的标志是存在抗TBM抗体(抗TBM-Ab)和密集的单核细胞浸润。使用在典型易感布朗挪威大鼠中生成的22种抗TBM单抗文库分析了该疾病中的抗TMB B细胞库。这些抗TBM单克隆抗体均被证明具有3M-1特异性,其特征构成了以下观察的基础:(a)估计有58个不同克隆的抗TBM B细胞群的大小; (b)根据竞争性抑制标准,所有抗TBM单抗都识别3M-1上相同(或在空间上接近)的表位。尽管亲和力有很大的变化,但仍保持了这种集中的识别。在患有抗TBM疾病的患者的人多克隆抗TBM抗血清中也可以证明抗原决定性优势。 (c)有交叉反应的独特型记录在案,针对这组可变区决定簇的抗血清被证明是预防疾病的有效方案,也是阻止疾病进展的治疗方法; (d)对VH基因家族的分析表明,尽管在抗TBM-Ab应答中使用了至少三个基因家族,但Q52和7183样家族的使用偏颇。因此,BN大鼠中的抗TBM B细胞区室中等大小,但主要集中于生肾抗原上的单个表位,并与疾病缓解型交叉反应性独特型有关。

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