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致肾炎性狼疮自身抗体的结构特征。

Structural features of nephritogenic lupus autoantibodies.

作者信息

Vargas M T, Gustilo K, D'Andrea D M, Kalluri R, Foster M H, Madaio M P

机构信息

Department of Medicine and The Penn Kidney Research Foundation, The University of Pennsylvania School of Medicine, Philadelphia 19104-6144, USA.

出版信息

Methods. 1997 Jan;11(1):62-9. doi: 10.1006/meth.1996.0388.

Abstract

We have identified monoclonal antibodies derived from MRL-lpr/lpr lupus-prone mice that produced nephritis after passive transfer to normal mice. Our present goal was to elucidate the structural and immunochemical features of nephritogenic Ig that facilitate immune deposition. For this purpose the antigen binding properties, capacity to form immune deposits, and nucleotide sequence of a genetically related autoantibody subgroup were compared. The prototype, H147 (an IgG encoded by 7183/81X VH gene), produced glomerular and tubular basement membrane, mesangial immune deposits, and proliferative glomerulonephritis after passive transfer to normal mice. For comparison three other 7183/81X encoded anti-DNA IgG (H257, H171, and H8a) were evaluated (predicted heavy chain aa homology >75%). H257 produced similar types of immune deposits as H147, and this was associated with nephritis; H8a produced predominantly mesangial deposits, whereas H171 did not produce significant deposits. Although their antigen binding profile to a panel of soluble autoantigens was variable, only H147 and H257 bound to both mesangial and aortic endothelial cell surfaces. V gene sequence analysis of the IgG suggests that individual residues, motifs, and conformations influence the autoantigen binding specificities that contributed to the observed differences in immune deposit formation.

摘要

我们已经鉴定出源自MRL-lpr/lpr狼疮易感小鼠的单克隆抗体,这些抗体在被动转移至正常小鼠后会引发肾炎。我们目前的目标是阐明致肾炎性免疫球蛋白的结构和免疫化学特征,这些特征有助于免疫复合物的沉积。为此,我们比较了一个基因相关的自身抗体亚组的抗原结合特性、形成免疫复合物的能力以及核苷酸序列。原型抗体H147(一种由7183/81X VH基因编码的IgG)在被动转移至正常小鼠后,会产生肾小球和肾小管基底膜、系膜免疫复合物沉积以及增殖性肾小球肾炎。为作比较,我们评估了另外三种由7183/81X编码的抗DNA IgG(H257、H171和H8a)(预测重链氨基酸同源性>75%)。H257产生与H147相似类型的免疫复合物沉积,且这与肾炎相关;H8a主要产生系膜沉积物,而H171未产生显著沉积物。尽管它们对一组可溶性自身抗原的抗原结合谱各不相同,但只有H147和H257能与系膜和主动脉内皮细胞表面结合。对这些IgG的V基因序列分析表明,个别残基、基序和构象会影响自身抗原结合特异性,这导致了观察到的免疫复合物形成差异。

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