Hilgendorff Anne, Windhorst Anita, Klein Manuel, Tchatalbachev Svetlin, Windemuth-Kieselbach Christine, Kreuder Joachim, Heckmann Matthias, Gkatzoflia Anna, Ehrhardt Harald, Mysliwietz Josef, Maier Michael, Izar Benjamin, Billion Andre, Gortner Ludwig, Chakraborty Trinad, Hossain Hamid
Department of Neonatology, Grosshadern, Ludwig-Maximilian University Munich, Germany and the Comprehensive Pneumology Center, Helmholtz Zentrum Muenchen, Munich, Germany, Member of the German Center for Lung Research (DZL), Munich, Germany.
Department of Pediatrics and Neonatology, Justus-Liebig University Giessen, Germany, Member of the German Center for Lung Research (DZL), Giessen, Germany.
J Mol Med (Berl). 2017 Feb;95(2):169-180. doi: 10.1007/s00109-016-1466-4. Epub 2016 Aug 30.
Early onset infection (EOI) in preterm infants <32 weeks gestational age (GA) is associated with a high mortality rate and the development of severe acute and long-term complications. The pathophysiology of EOI is not fully understood and clinical and laboratory signs of early onset infections in this patient cohort are often not conclusive. Thus, the aim of this study was to identify signatures characterizing preterm infants with EOI by using genome-wide gene expression (GWGE) analyses from umbilical arterial blood of preterm infants. This prospective cohort study was conducted in preterm infants <32 weeks GA. GWGE analyses using CodeLink human microarrays were performed from umbilical arterial blood of preterm infants with and without EOI. GWGE analyses revealed differential expression of 292 genes in preterm infants with EOI as compared to infants without EOI. Infants with EOI could be further differentiated into two subclasses and were distinguished by the magnitude of the expression of genes involved in both neutrophil and T cell activation. A hallmark activity for both subclasses of EOI was a common suppression of genes involved in natural killer (NK) cell function, which was independent from NK cell numbers. Significant results were recapitulated in an independent validation cohort. Gene expression profiling may enable early and more precise diagnosis of EOI in preterm infants.
Gene expression (GE) profiling at birth characterizes preterm infants with EOI. GE analysis indicates dysregulation of NK cell activity. NK cell activity at birth may be a useful marker to improve early diagnosis of EOI.
孕周小于32周的早产儿早发型感染(EOI)与高死亡率以及严重急性和长期并发症的发生有关。EOI的病理生理学尚未完全了解,该患者队列中早发型感染的临床和实验室体征往往不具有决定性。因此,本研究的目的是通过对早产儿脐动脉血进行全基因组基因表达(GWGE)分析,确定表征EOI早产儿的特征。这项前瞻性队列研究在孕周小于32周的早产儿中进行。使用CodeLink人类微阵列对有和没有EOI的早产儿脐动脉血进行GWGE分析。GWGE分析显示,与没有EOI的婴儿相比,有EOI的早产儿中有292个基因表达存在差异。患有EOI的婴儿可进一步分为两个亚类,并通过参与中性粒细胞和T细胞激活的基因表达程度来区分。EOI两个亚类的一个标志性活动是共同抑制参与自然杀伤(NK)细胞功能的基因,这与NK细胞数量无关。在一个独立的验证队列中重现了显著结果。基因表达谱分析可能有助于对早产儿EOI进行早期和更精确的诊断。
出生时的基因表达(GE)谱可表征患有EOI的早产儿。GE分析表明NK细胞活性失调。出生时的NK细胞活性可能是改善EOI早期诊断的有用标志物。
Zotero 插件
