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预测鼠类和人类宿主对典型和非典型肺炎反应的特征。

Predictive signature of murine and human host response to typical and atypical pneumonia.

机构信息

Department of Medicine, Duke University School of Medicine, Durham, North Carolina, USA

Department of Medicine, Duke University School of Medicine, Durham, North Carolina, USA.

出版信息

BMJ Open Respir Res. 2024 Aug 3;11(1):e002001. doi: 10.1136/bmjresp-2023-002001.

Abstract

BACKGROUND

Pneumonia due to typical bacterial, atypical bacterial and viral pathogens can be difficult to clinically differentiate. Host response-based diagnostics are emerging as a complementary diagnostic strategy to pathogen detection.

METHODS

We used murine models of typical bacterial, atypical bacterial and viral pneumonia to develop diagnostic signatures and understand the host's response to these types of infections. Mice were intranasally inoculated with , , influenza or saline as a control. Peripheral blood gene expression analysis was performed at multiple time points. Differentially expressed genes were used to perform gene set enrichment analysis and generate diagnostic signatures. These murine-derived signatures were externally validated in silico using human gene expression data. The response to was the most rapid and robust.

RESULTS

Mice infected with had a delayed response more similar to influenza-infected animals. Diagnostic signatures for the three types of infection had 0.94-1.00 area under the receiver operator curve (auROC). Validation in five human gene expression datasets revealed auROC of 0.82-0.96.

DISCUSSION

This study identified discrete host responses to typical bacterial, atypical bacterial and viral aetiologies of pneumonia in mice. These signatures validated well in humans, highlighting the conserved nature of the host response to these pathogen classes.

摘要

背景

由典型细菌、非典型细菌和病毒病原体引起的肺炎在临床上难以区分。基于宿主反应的诊断方法作为一种病原体检测的补充诊断策略正在出现。

方法

我们使用典型细菌、非典型细菌和病毒性肺炎的小鼠模型来开发诊断特征,并了解宿主对这些类型感染的反应。小鼠通过鼻腔内接种 、 、流感或生理盐水作为对照进行感染。在多个时间点进行外周血基因表达分析。差异表达基因用于进行基因集富集分析并生成诊断特征。这些从鼠类中获得的特征通过使用人类基因表达数据进行了计算机模拟的外部验证。 感染的反应最为迅速和强烈。

结果

感染 的小鼠反应延迟,与感染流感的动物更为相似。三种感染类型的诊断特征具有 0.94-1.00 的接收器操作特征曲线下面积(auROC)。在五个人类基因表达数据集的验证中,auROC 为 0.82-0.96。

讨论

本研究在小鼠中确定了针对典型细菌、非典型细菌和病毒性肺炎病因的离散宿主反应。这些特征在人类中得到了很好的验证,突出了宿主对这些病原体类别的反应的保守性质。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9e1e/11298752/40666937901e/bmjresp-11-1-g001.jpg

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