促炎细胞因子比率决定接受化疗的儿童发热性中性粒细胞减少症的临床病程。

IF 2.4 Q1 PEDIATRICS
Mira Siegmund, Julia Pagel, Tasja Scholz, Jan Rupp, Christoph Härtel, Melchior Lauten
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引用次数: 0

摘要

背景:发热性中性粒细胞减少症是儿童癌症治疗过程中常见且严重的并发症。经验广谱抗生素通常使用,直到中性粒细胞计数恢复。本研究的目的是利用体外脓毒症模型来研究细胞因子谱作为潜在的生物标志物,以区分发热性中性粒细胞减少症(FN)的不同临床病程。方法:我们对小儿肿瘤患者FN发作进行了一项观察性研究。中性粒细胞减少的病程被定义为严重的情况下,证实血流感染或临床证据的复杂感染。我们在FN发作后的不同时间点采集血液样本,并用脂多糖(LPS)和表皮葡萄球菌(SE)刺激体外24小时。通过多重免疫分析系统测量全血培养上清中27种细胞因子的水平。结果:调查了33例儿童47例FN发作。随着时间的推移,IL-8、IL-1β和MCP-1的表达显著增加。IL-8、MIP-1α、MIP-1β、MCP-1和TNF-α浓度在FN临床严重病程患者中显著降低。结论:细胞因子谱的不同模式似乎能够确定感染性FN并预测其临床病程的严重程度。如果这些数据可以在多中心环境中得到验证,这可能最终导致个性化的治疗策略,促进这些患者的抗生素管理。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Pro-inflammatory cytokine ratios determine the clinical course of febrile neutropenia in children receiving chemotherapy.

Pro-inflammatory cytokine ratios determine the clinical course of febrile neutropenia in children receiving chemotherapy.

Pro-inflammatory cytokine ratios determine the clinical course of febrile neutropenia in children receiving chemotherapy.

Background: Febrile neutropenia is a common and serious complication during treatment of childhood cancer. Empirical broad-spectrum antibiotics are usually administered until neutrophil cell count recovery. It was the aim of this study to investigate cytokine profiles as potential biomarkers using in-vitro sepsis models to differentiate between distinct clinical courses of febrile neutropenia (FN).

Methods: We conducted an observational study in FN episodes of pediatric oncology patients. Courses of neutropenia were defined as severe in case of proven blood stream infection or clinical evidence of complicated infection. We collected blood samples at various time points from the onset of FN and stimulated ex vivo with lipopolysaccharide (LPS) and Staphylococcus epidermidis (SE) for 24 h. Twenty-seven cytokine levels were measured in the whole blood culture supernatants by a multiplex immunoassay system.

Results: Forty-seven FN episodes from 33 children were investigated. IL-8, IL-1β, and MCP-1 expression increased significantly over time. IL-8, MIP-1α, MIP-1β, MCP-1, and TNF-α showed significantly lower concentration in patients with a clinically severe course of the FN.

Conclusions: Distinct patterns of cytokine profiles seem to be able to determine infectious FN and to predict the severity of its clinical course. If these data can be verified in a multi-centre setting, this may finally lead to an individualized treatment strategy facilitating antibiotic stewardship in these patients.

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