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Emerging trends in Lassa fever: redefining the role of immunoglobulin M and inflammation in diagnosing acute infection

机译:拉沙热的新兴趋势:重新定义免疫球蛋白M和炎症在诊断急性感染中的作用

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Background Lassa fever (LF) is a devastating hemorrhagic viral disease that is endemic to West Africa and responsible for thousands of human deaths each year. Analysis of humoral immune responses (IgM and IgG) by antibody-capture ELISA (Ab-capture ELISA) and Lassa virus (LASV) viremia by antigen-capture ELISA (Ag-capture ELISA) in suspected patients admitted to the Kenema Government Hospital (KGH) Lassa Fever Ward (LFW) in Sierra Leone over the past five years is reshaping our understanding of acute LF. Results Analyses in LF survivors indicated that LASV-specific IgM persists for months to years after initial infection. Furthermore, exposure to LASV appeared to be more prevalent in historically non-endemic areas of West Africa with significant percentages of reportedly healthy donors IgM and IgG positive in LASV-specific Ab-capture ELISA. We found that LF patients who were Ag positive were more likely to die than suspected cases who were only IgM positive. Analysis of metabolic and immunological parameters in Ag positive LF patients revealed a strong correlation between survival and low levels of IL-6, -8, -10, CD40L, BUN, ALP, ALT, and AST. Despite presenting to the hospital with fever and in some instances other symptoms consistent with LF, the profiles of Ag negative IgM positive individuals were similar to those of normal donors and nonfatal (NF) LF cases, suggesting that IgM status cannot necessarily be considered a diagnostic marker of acute LF in suspected cases living in endemic areas of West Africa. Conclusion Only LASV viremia assessed by Ag-capture immunoassay, nucleic acid detection or virus isolation should be used to diagnose acute LASV infection in West Africans. LASV-specific IgM serostatus cannot be considered a diagnostic marker of acute LF in suspected cases living in endemic areas of West Africa. By applying these criteria, we identified a dysregulated metabolic and pro-inflammatory response profile conferring a poor prognosis in acute LF. In addition to suggesting that the current diagnostic paradigm for acute LF should be reconsidered, these studies present new opportunities for therapeutic interventions based on potential prognostic markers in LF.
机译:背景技术拉萨热(LF)是一种毁灭性的出血性病毒病,在西非流行,每年造成数千人死亡。通过抗体捕获ELISA(Ab捕获ELISA)和拉萨病毒(LASV)病毒血症通过抗原捕获ELISA(Ag捕获ELISA)分析可疑患者进入凯内玛政府医院(KGH)的体液免疫应答(IgM和IgG) )过去五年来塞拉利昂的拉萨热病房(LFW)正在重塑我们对急性LF的理解。结果LF幸存者的分析表明,LASV特异性IgM在初次感染后持续数月至数年。此外,在西非的历史非流行地区,暴露于LASV的情况似乎更为普遍,据报道,在LASV特异性Ab捕获ELISA中,有相当比例的据报告健康的供体IgM和IgG阳性。我们发现,Ag阳性的LF患者比仅IgM阳性的可疑病例更有可能死亡。 Ag阳性LF患者的代谢和免疫学参数分析显示,存活率与低水平的IL-6,-8,-10,CD40L,BUN,ALP,ALT和AST密切相关。尽管在医院出现发烧以及在某些情况下出现其他与LF一致的症状,但Ag阴性的IgM阳性个体的特征与正常供体和非致命(NF)LF病例相似,这表明IgM的状况不一定被认为是诊断性的居住在西非流行地区的疑似病例中急性LF的标志物。结论只有通过Ag捕获免疫分析,核酸检测或病毒分离评估的LASV病毒血症才可用于诊断西非人的急性LASV感染。在居住于西非流行地区的可疑病例中,不能将LASV特异性IgM血清状况视为急性LF的诊断标志。通过应用这些标准,我们确定了代谢异常和促炎反应谱失调,从而导致急性LF的不良预后。除了建议重新考虑当前急性LF的诊断模式外,这些研究还根据LF的潜在预后标志物提供了治疗干预的新机会。

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