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特发性肺纤维化中自身抗体识别的拓扑异构酶IIα表位图谱

Mapping of topoisomerase II alpha epitopes recognized by autoantibodies in idiopathic pulmonary fibrosis.

作者信息

Grigolo B, Mazzetti I, Borzì R M, Hickson I D, Fabbri M, Fasano L, Meliconi R, Facchini A

机构信息

Laboratorio di Immunologia e Genetica, Istituto di Ricerca Codivilla Putti, Istituti Ortopedici Rizzoli (I.O.R.), Bologna, Italy.

出版信息

Clin Exp Immunol. 1998 Dec;114(3):339-46. doi: 10.1046/j.1365-2249.1998.00747.x.

Abstract

Autoantibodies against DNA topoisomerase II alpha have been identified in the sera of patients with idiopathic pulmonary fibrosis (IPF). To map topoisomerase II autoepitopes, we tested by ELISA and immunoblotting the IPF anti-topoisomerase II-positive sera against a series of recombinant proteins which covered the full length of topoisomerase II alpha. Specific patterns of reactivity were observed, indicating the existence of multiple epitopes on topoisomerase II, either highly complex or conformational/discontiguous or conformational/contiguous ones. The latter resided in amino acid residues 854-1147 and 1370-1447. A detailed analysis of these regions was undertaken, but we were not able to pinpoint a sequential peptide-sized epitope, or any significant homology with foreign pathogens. Further, we observed a significant correlation between the progression from a contiguous to a quaternary/tertiary structure-dependent autoepitope and the disease duration but not with the disease severity. Therefore, this result supports the hypothesis that anti-topoisomerase II autoreactivity evolves following an antigen-driven process.

摘要

在特发性肺纤维化(IPF)患者的血清中已鉴定出针对DNA拓扑异构酶IIα的自身抗体。为了绘制拓扑异构酶II自身表位图谱,我们通过酶联免疫吸附测定(ELISA)和免疫印迹法,用一系列覆盖拓扑异构酶IIα全长的重组蛋白检测IPF抗拓扑异构酶II阳性血清。观察到了特异性反应模式,表明拓扑异构酶II上存在多个表位,这些表位要么高度复杂,要么是构象性/不连续的,要么是构象性/连续的。后者位于氨基酸残基854 - 1147和1370 - 1447处。我们对这些区域进行了详细分析,但未能确定一个连续的肽大小的表位,也未发现与外来病原体有任何显著同源性。此外,我们观察到从连续表位向四级/三级结构依赖性自身表位的转变与疾病持续时间之间存在显著相关性,但与疾病严重程度无关。因此,这一结果支持了抗拓扑异构酶II自身反应性是在抗原驱动过程之后演变而来的这一假说。

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