首页> 外文期刊>Disease markers >Antibodies against 4-hydroxy-2-nonenal modified epitopes recognized chromatin and its oxidized forms: Role of chromatin, oxidized forms of chromatin and 4-hydroxy-2-nonenal modified epitopes in the etiopathogenesis of SLE
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Antibodies against 4-hydroxy-2-nonenal modified epitopes recognized chromatin and its oxidized forms: Role of chromatin, oxidized forms of chromatin and 4-hydroxy-2-nonenal modified epitopes in the etiopathogenesis of SLE

机译:针对4-羟基-2-壬烯修饰的抗原表位的抗体识别染色质及其氧化形式:染色质,染色质的氧化形式和4-羟基-2-壬烯修饰的抗原表位在SLE的发病机制中的作用

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Objectives: This study was undertaken to investigate the role of lipid oxidative-by-product 4-hydroxy-2-nonenal (HNE)-modified human serum albumin (HSA), chromatin, reactive oxygen species (ROS)-modified chromatin and nitric oxide (NO)-modified chromatin in systemic lupus erythematosus (SLE). Methods: HSA was modified by HNE. Immunogenicity of modified HSA was probed by inducing polyclonal antibodies in rabbits. Chromatin was isolated from goat liver and modified by ROS or NO. Immunocross-reactions of Protein-A purified anti-HNE-HSA-IgG with chromatin, ROS-chromatin and NO-chromatin were determined. Autoantibodies from 74 SLE patients were screened. HSA was isolated from SLE patients (SLE-HSA) and immunocross-reactions of isolated SLE-HSA with HNE-specific antibodies were investigated. Results: HNE-HSA was found to be highly immunogenic in rabbits. The notable feature of anti-HNE-HSA-IgG showed cross-reactions with chromatin, ROS-chromatin and NO-chromatin (p< 0.01). High degree of specific binding to HNE-HSA, chromatin, ROS-chromatin or NO-chromatin was observed with antibodies from 55% of SLE patients. SLE anti-native/ oxidized chromatin antibodies showed specificity towards HNE-HSA. Furthermore, SLE-HSA showed binding with HNE-specific antibodies. Conclusions: This is the first study to demonstrate that chromatin and its oxidized forms have been recognized by antibodies against HNE modified epitopes. Our results provide an important insight into the immunological basis of the reported HNE-modified epitopes in SLE.
机译:目的:本研究旨在研究脂质氧化副产物4-羟基-2-壬烯(HNE)修饰的人血清白蛋白(HSA),染色质,活性氧(ROS)修饰的染色质和一氧化氮的作用。 (NO)修饰的系统性红斑狼疮(SLE)中的染色质。方法:用HNE对HSA进行修饰。通过在兔中诱导多克隆抗体来探测修饰的HSA的免疫原性。从山羊肝脏中分离出染色质,并通过ROS或NO对其进行了修饰。确定了蛋白A纯化的抗HNE-HSA-IgG与染色质,ROS染色质和NO染色质的免疫交叉反应。筛选了74名SLE患者的自身抗体。从SLE患者中分离出HSA(SLE-HSA),并研究分离出的SLE-HSA与HNE特异性抗体的免疫交叉反应。结果:发现HNE-HSA在兔中具有高度免疫原性。抗HNE-HSA-IgG的显着特征是与染色质,ROS-染色质和NO-染色质发生交叉反应(p <0.01)。使用55%的SLE患者的抗体观察到与HNE-HSA,染色质,ROS-染色质或NO-染色质的高度特异性结合。 SLE抗天然/氧化染色质抗体表现出对HNE-HSA的特异性。此外,SLE-HSA显示与HNE特异性抗体结合。结论:这是第一项证明染色质及其氧化形式已被抗HNE修饰表位的抗体识别的研究。我们的结果为SLE中报道的HNE修饰表位的免疫学基础提供了重要的见识。

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