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首页> 外文期刊>The journal of immunology >Immunoproteomic Identification and Serological Responses to Novel Chlamydia pneumoniae Antigens That Are Associated with Persistent C. pneumoniae Infections
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Immunoproteomic Identification and Serological Responses to Novel Chlamydia pneumoniae Antigens That Are Associated with Persistent C. pneumoniae Infections

机译:免疫性与永久性肺炎衣原体感染相关的新型肺炎衣原体抗原的免疫学鉴定和血清学反应。

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The controversial discussion about the role of Chlamydia pneumoniae in atherosclerosis cannot be solved without a reliable diagnosis that allows discrimination between past and persistent infections. Using a proteomic approach and immunoblotting with human sera, we identified 31 major C. pneumoniae Ags originating from 27 different C. pneumoniae proteins. More than half of the proteins represent Chlamydia Ags not described previously. Using a comparative analysis of spot reactivity Pmp6, OMP2, GroEL, DnaK, RpoA, EF-Tu, as well as CpB0704 and CpB0837, were found to be immunodominant. The comparison of Ab-response patterns of sera from subjects with and without evidence for persisting C. pneumoniae , determined by multiple PCR analysis of PBMC and vasculatory samples, resulted in differential reactivity for 12 proteins, which is not reflected by reactivity of the sera in the microimmunofluorescence test, the current gold standard for serodiagnosis. Although reactivity of sera from PCR-positive donors was increased toward RpoA, MOMP, YscC, Pmp10, PorB, Pmp21, GroEL, and Cpaf, the reactivity toward YscL, Rho, LCrE, and CpB0837 was decreased, reflecting the altered protein expression of persisting C. pneumoniae in vitro. Our data provide the first evidence of a unique Ab-response pattern associated with persistent C. pneumoniae infections, which is a prerequisite for the serological determination of persistently infected patients.
机译:如果没有可靠的诊断方法能够区分过去和持续的感染,就无法解决有关肺炎衣原体在动脉粥样硬化中作用的争议性讨论。使用蛋白质组学方法并用人血清进行免疫印迹,我们鉴定了源自27种不同的肺炎衣原体蛋白的31种主要肺炎衣原体Ags。超过一半的蛋白质代表衣原体Ags,以前没有描述。通过对斑点反应性进行比较分析,发现Pmp6,OMP2,GroEL,DnaK,RpoA,EF-Tu以及CpB0704和CpB0837具有免疫优势。通过对PBMC和脉管系统样品进行多重PCR分析确定的有和没有肺炎衣原体持续存在证据的受试者的血清Ab反应模式的比较,导致12种蛋白质的反应性差异,而血清中的反应性并未反映该差异。微量免疫荧光测试,当前血清学诊断的金标准。尽管来自PCR阳性供体的血清对RpoA,MOMP,YscC,Pmp10,PorB,Pmp21,GroEL和Cpaf的反应性增加,但对YscL,Rho,LCrE和CpB0837的反应性却降低了,反映了持久性蛋白表达的改变体外肺炎衣原体。我们的数据提供了与持续性肺炎衣原体感染相关的独特Ab反应模式的第一个证据,这是确定持续感染患者进行血清学检测的前提。

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