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Markers of neutrophil activation and extracellular traps formation are predictive of appendicitis in mice and humans: a pilot study

机译:中性粒细胞激活和细胞外疏水膜形成的标记是小鼠和人类的阑尾炎的预测:试点研究

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摘要

Abstract Appendicitis is one of the most frequent emergencies in pediatric surgery, yet current biomarkers for diagnosis are unspecific and have low predictive values. As neutrophils and extracellular traps (ETs) are an essential component of the immune defense against bacterial infections, and appendicitis is considered an inflammation reaction of the appendix, we hypothesized that neutrophil activation and NET formation play an essential role in appendicitis development and maintenance. Therefore, this pilot study aimed to establish a murine model of appendicitis and to evaluate ETs markers to diagnose appendicitis in mice and humans. The study used 20 (12 appendicitis- and 8 controls) 6-week old mice which underwent advanced appendicitis induction using a modified caecal ligation puncture procedure. During the study, cell-free DNA, neutrophil elastase (NE), myeloperoxidase (MPO), and citrullinated Histone H3 (H3cit) were assessed. Additionally, samples of 5 children with histologically confirmed appendicitis and 5 matched controls with catarrhal appendicitis, were examined for the same biomarkers. Moreover, NE, MPO, and H3cit were assessed histologically via immunofluorescence in mice and humans. All mice in the appendicitis group developed an advanced form of appendicitis with focal peritonitis. In mice and humans with appendicitis, markers of neutrophil activation and ETs formation (especially cfDNA, NE and H3cit) were significantly elevated in blood and tissue compared to controls. Ultimately, biomarkers correlated extremely well with tissue expression and thus disease severity. It appears that neutrophil activation and possibly NETs contribute to appendicitis development and biomarkers of neutrophil activation and ET formation reflect disease severity and thus could be used as biomarkers for appendicitis. However, large prospective clinical studies are needed to confirm our findings.
机译:摘要阑尾炎是儿科手术中最常见的紧急情况之一,但目前的诊断生物标志物是未指定的并且具有低预测值。作为中性粒细胞和细胞外疏水膜(ETS)是免疫防御免疫防御的重要组成部分,并且阑尾炎被认为是附录的炎症反应,我们假设中性粒细胞激活和净形成在阑尾炎开发和维护中起重要作用。因此,该试点研究旨在建立阑尾炎的小鼠模型,并评估ETS标记以诊断小鼠和人类的阑尾炎。该研究使用了20名(12个阑尾炎和8个对照)6周龄小鼠,使用改良的颈部结扎穿刺程序进行高级阑尾炎诱导。在研究期间,评估无细胞DNA,中性粒细胞弹性蛋白酶(NE),髓过氧化物酶(MPO)和瓜氨酸组蛋白H3(H3Cit)。另外,针对同一生物标志物检查了5名具有组织学证实的阑尾炎和5种匹配对照的儿童的样品。此外,通过小鼠和人类的免疫荧光组织地评估NE,MPO和H 3Cit。阑尾炎组的所有小鼠都开发出一种先进形式的阑尾炎,具有焦腹膜炎。在小鼠和具有阑尾炎的人类中,与对照相比,血液和组织中,中性粒细胞激活和ETS形成的标记(特别是CFDNA,NE和H3Cit)显着升高。最终,生物标志物与组织表达相比,疾病严重程度非常好。似乎中性粒细胞激活和可能净的蚊帐有助于中性粒细胞激活的阑尾炎和生物标志物,ET形成反映疾病严重程度,因此可以用作阑尾炎的生物标志物。然而,需要大型前瞻性临床研究来确认我们的研究结果。

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