Author: Hermann, Stefanie; Brandes, Florian; Kirchner, Benedikt; Buschmann, Dominik; Borrmann, Melanie; Klein, Matthias; Kotschote, Stefan; Bonin, Michael; Reithmair, Marlene; Kaufmann, Ines; Schelling, Gustav; Pfaffl, Michael W.
Title: Diagnostic potential of circulating cellâ€free microRNAs for communityâ€acquired pneumonia and pneumoniaâ€related sepsis Cord-id: cgchvsq2 Document date: 2020_9_11
ID: cgchvsq2
Snippet: Cellâ€free microRNAs (miRNAs) are transferred in disease state including inflammatory lung diseases and are often packed into extracellular vesicles (EVs). To assess their suitability as biomarkers for communityâ€acquired pneumonia (CAP) and severe secondary complications such as sepsis, we studied patients with CAP (n = 30), sepsis (n = 65) and healthy volunteers (n = 47) subdivided into a training (n = 67) and a validation (n = 75) cohort. After precipitating crude EVs from sera, associated
Document: Cellâ€free microRNAs (miRNAs) are transferred in disease state including inflammatory lung diseases and are often packed into extracellular vesicles (EVs). To assess their suitability as biomarkers for communityâ€acquired pneumonia (CAP) and severe secondary complications such as sepsis, we studied patients with CAP (n = 30), sepsis (n = 65) and healthy volunteers (n = 47) subdivided into a training (n = 67) and a validation (n = 75) cohort. After precipitating crude EVs from sera, associated small RNA was profiled by nextâ€generation sequencing (NGS) and evaluated in multivariate analyses. A subset of the thereby identified biomarker candidates was validated both technically and additionally by reverse transcription quantitative realâ€time PCR (RTâ€qPCR). Differential gene expression (DGE) analysis revealed 29 differentially expressed miRNAs in CAP patients when compared to volunteers, and 25 miRNAs in patients with CAP, compared to those with sepsis. Sparse partialâ€least discriminant analysis separated groups based on 12 miRNAs. Three miRNAs proved as a significant biomarker signature. While expression levels of miRâ€1246 showed significant changes with an increase in overall disease severity from volunteers to CAP and to sepsis, miRâ€193aâ€5p and miRâ€542â€3p differentiated patients with an infectious disease (CAP or sepsis) from volunteers. Cellâ€free miRNAs are potentially novel biomarkers for CAP and may help to identify patients at risk for progress to sepsis, facilitating early intervention and treatment.
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