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首页> 外文期刊>Scandinavian journal of immunology. >Two nuclear dot-associated proteins, PML and Sp100, are often co-autoimmunogenic in patients with primary biliary cirrhosis.
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Two nuclear dot-associated proteins, PML and Sp100, are often co-autoimmunogenic in patients with primary biliary cirrhosis.

机译:在原发性胆汁性肝硬化患者中,两种核点相关蛋白PML和Sp100通常具有共同自身免疫原性。

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The nucleoproteins Sp100 and PML, the first an autoantigen predominant in patients with primary biliary cirrhosis (PBC) and the second a transformation and cell growth suppressing protein aberrantly expressed in promyelocytic leukaemia cells, were recently shown to colocalize in dot-like nuclear domains. Here we analysed whether PML, like Sp100, is also an autoantigen in patients with PBC and other autoimmune diseases, and wether both proteins interact directly. Testing sera from autoimmune patients using an immunoprecipitation assay with radiolabelled PML and an immunofluorescence assay based on a cell line overexpressing PML, autoantibodies (Aabs) against PML were found in the majority o anti-Sp100 Aab positive patients. Only very few patients with PBC or other autoimmune diseases contained anti-PML or anti-Sp100 Aabs exclusively. In contrast to Sp100, immunoreactivity of recombinant PML in immunoblots was only weak and was directed to one region. This suggests that anti-PML Aabs recognize fewer and preferentially conformation-dependent epitopes. In an immunoprecipitation assay using in vitro synthesized Sp100 and PML proteins and Abs to recombinant proteins, no direct interaction was observed. Taken together, these data indicate that Aabs against PML are as highly prevalent and specific for patients with PBC as those against Sp100. The colocalization of these autoantigens and the frequent co-occurrence of the corresponding Aabs might reflect an association of both proteins mediated by one or several other proteins.
机译:最近显示,核蛋白Sp100和PML是第一个在原发性胆汁性肝硬化(PBC)患者中占主导地位的自身抗原,第二个是在早幼粒细胞白血病细胞中异常表达的转化和细胞生长抑制蛋白,它们在点状核域中共定位。在这里,我们分析了PML是否像Sp100一样也是PBC和其他自身免疫性疾病患者的自身抗原,并且这两种蛋白是否直接相互作用。使用带有放射性标记的PML的免疫沉淀测定法和基于过度表达PML的细胞系的免疫荧光测定法测试自身免疫患者的血清,在大多数抗Sp100 Aab阳性的患者中发现了针对PML的自身抗体(Aabs)。只有极少数患有PBC或其他自身免疫性疾病的患者专门含有抗PML或抗Sp100 Aab。与Sp100相比,重组PML在免疫印迹中的免疫反应性很弱,仅针对一个区域。这表明抗PML Aabs识别较少且优先依赖构象的表位。在使用体外合成的Sp100和PML蛋白以及Abs重组蛋白进行的免疫沉淀测定中,未观察到直接相互作用。综上所述,这些数据表明,针对PML的Aab与针对Sp100的Aab一样,对PBC患者同样普遍。这些自身抗原的共定位和相应Aab的频繁共存可能反映了由一种或几种其他蛋白质介导的两种蛋白质的关联。

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