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Development of a Novel Inhalational Model of Invasive Pulmonary Aspergillosis in Rats and Comparative Evaluation of Three Biomarkers for Its Diagnosis

机译:新型大鼠侵袭性肺曲霉菌吸入模型的建立及三种生物标志物的诊断比较评价

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摘要

Aspergillus fumigatus, a thermotolerant fungus, is the main causative agent of invasive pulmonary aspergillosis (IPA) in immunocompromised patients that is associated with high mortality rates. Early diagnosis of IPA is crucial for mortality reduction and improved prognosis. An experimental inhalational model of IPA was developed in rats and the efficacy of three biomarkers, namely β-D-glucan (BDG), a panfungal marker, galactomannan (GM), a genus-specific marker, and A. fumigatus DNA, a species-specific marker was evaluated in serum and bronchoalveolar lavage (BAL) specimens at different time points postinfection for early diagnosis of IPA. BDG and GM were detected by using commercial Fungitell and Platelia Aspergillus EIA kits, respectively. A. fumigatus DNA was detected by developing a sensitive, single-step PCR assay. IPA was successfully developed in immunosuppressed rats and all animals until 5 days post-infection were positive for A. fumigatus by culture and KOH-calcofluor microscopy also showed A. fumigatus in 19 of 24 (79%) lung tissue samples. Fourteen of 30 (47%) and 27 of 30 (90%) serum and BAL specimens, respectively, were positive for all three biomarkers with 100% specificity (none of sera or BAL specimens of 12 control rats was positive for biomarkers). Our data show that BAL is a superior specimen than serum and combined detection of BDG, GM and A. fumigatus DNA provide a sensitive diagnosis of IPA in an experimental animal model. Moreover, combined detection of GM and DNA in BAL and detection of either GM or DNA in serum was also positive in 27 of 30 (90%) animals. For economic reasons and considering that the positive predictive value of BDG is low, the detection of GM and/or DNA in serum and BAL samples has the potential to serve as an integral component of the diagnostic-driven strategy in high-risk patients suspected for IPA.
机译:烟曲霉是一种耐热真菌,是免疫力低下患者侵袭性肺曲霉病(IPA)的主要病因,与高死亡率相关。 IPA的早期诊断对于降低死亡率和改善预后至关重要。在大鼠中建立了IPA的实验性吸入模型,并使用了三种生物标记物,即β-D-葡聚糖(BDG),泛真菌标记物,半乳甘露聚糖(GM)(属特异性标记物)和烟曲霉DNA(一种物种)的功效。在感染后不同时间点在血清和支气管肺泡灌洗(BAL)标本中评估特异性标记,以早期诊断IPA。使用商业的Fungitell和Platelia Aspergillus EIA试剂盒分别检测了BDG和GM。烟曲霉DNA通过开发敏感的单步PCR测定法进行检测。在免疫抑制的大鼠中成功开发了IPA,直到感染后5天为止,所有动物的烟曲霉培养均呈阳性,KOH荧光显微镜还显示24个肺组织样品中有19个(79%)烟曲霉。 30种血清标志物和BAL标本分别在30个血清标志物和BAL标本中分别占30个样本中的14个(47%)和30个样本(90%)中27个呈阳性(12只对照大鼠的血清或BAL标本中没有一个对生物标志物呈阳性)。我们的数据表明,BAL比血清更优越,并且BDG,GM和烟曲霉DNA的联合检测可在实验动物模型中对IPA进行灵敏的诊断。此外,在30只动物中,有27只(90%)的BAL中GM和DNA的联合检测以及血清中GM或DNA的检测也是阳性的。出于经济原因,并考虑到BDG的阳性预测值较低,因此在血清和BAL样品中检测GM和/或DNA可能会成为疑似感染的高危患者诊断驱动策略的重要组成部分IPA。

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