首页> 美国卫生研究院文献>Journal of Clinical Microbiology >Immunoglobulin G Responses to a Panel of Candida albicans Antigens as Accurate and Early Markers for the Presence of Systemic Candidiasis
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Immunoglobulin G Responses to a Panel of Candida albicans Antigens as Accurate and Early Markers for the Presence of Systemic Candidiasis

机译:免疫球蛋白G对白色念珠菌抗原的反应是存在系统性念珠菌病的准确和早期标记

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摘要

Despite shortcomings, cultures of blood and sterile sites remain the “gold standard” for diagnosing systemic candidiasis. Alternative diagnostic markers, including antibody detection, have been developed, but none are widely accepted. In this study, we used an enzyme-linked immunosorbent assay to measure serum antibody responses against 15 recombinant Candida albicans antigens among 60 patients with systemic candidiasis due to various Candida spp. and 24 uninfected controls. Mean immunoglobulin G (IgG) responses against all 15 antigens were significantly higher among patients with systemic candidiasis than among controls, whereas IgM responses were higher against only seven antigens. Using discriminant analysis that included IgG responses against the 15 antigens, we derived a mathematical prediction model that identified patients with systemic candidiasis with an error rate of 3.7%, a sensitivity of 96.6%, and a specificity of 95.6%. Furthermore, a prediction model using a subset of four antigens (SET1, ENO1, PGK1-2, and MUC1-2) identified through backward elimination and canonical correlation analyses performed as accurately as the full panel. Using the simplified model, we predicted systemic candidiasis in a separate test sample of 32 patients and controls with 100% sensitivity and 87.5% specificity. We also demonstrated that IgG titers against each of the four antigens included in the prediction model were significantly higher in convalescent-phase sera than in paired acute-phase sera. Taken together, our findings suggest that IgG responses against a panel of candidal antigens might represent an accurate and early marker of systemic candidiasis, a hypothesis that should be tested in future trials.
机译:尽管存在缺陷,血液和无菌部位的培养仍是诊断系统性念珠菌病的“金标准”。已经开发了包括抗体检测在内的其他诊断标记,但没有一个被广泛接受。在这项研究中,我们使用酶联免疫吸附测定法测量了60名因各种念珠菌属引起的系统性念珠菌病患者中针对15种重组白色念珠菌抗原的血清抗体反应。和24个未感染的对照。系统性念珠菌病患者对所有15种抗原的平均免疫球蛋白G(IgG)应答均显着高于对照组,而仅对7种抗原的IgM应答较高。使用包括针对15种抗原的IgG应答在内的判别分析,我们得出了数学预测模型,该模型识别出患有系统性念珠菌病的患者,错误率为3.7%,敏感性为96.6%,特异性为95.6%。此外,通过反向消除和规范相关分析确定的使用四个抗原(SET1,ENO1,PGK1-2和MUC1-2)的子集的预测模型的准确度与全图一样。使用简化模型,我们以32%的患者和对照的单独测试样本预测了系统性念珠菌病,其敏感性为100%,特异性为87.5%。我们还证明,针对预测模型中包含的四种抗原中的每一种的IgG滴度在恢复期血清中均显着高于配对急性期血清。综上所述,我们的发现表明,针对一组念珠菌抗原的IgG应答可能代表了系统性念珠菌病的准确和早期标记,这一假说应在以后的试验中进行验证。

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