CD64 和髓过氧化物酶作为早期诊断儿科重症监护室败血症的生物标记物的作用。

Q3 Medicine
Heba M Ahmed, Eman M Ali, Karima S Abdelrhman, Dalia S Morgan, Nesreen M K Taha, Mahmoud Hodeib
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引用次数: 0

摘要

在全球范围内,败血症是导致儿童死亡的主要原因。虽然对成人进行的研究对新生儿和幼儿败血症的诊断和治疗有重要影响,但有一些重要因素也与儿科有关。这项前瞻性病例对照研究是在机构伦理委员会批准后,于 2020 年 8 月至 2022 年 10 月期间进行的。研究对象包括儿科重症监护室收治的 48 名重症患儿,以及作为对照组的 30 名表面健康的患儿。所有参与者均接受了实验室检查,包括全血细胞计数、C反应蛋白(CRP)、血液培养、分化簇64(CD64)和髓过氧化物酶(MPO)的敏感性和血浆水平。对全身炎症反应综合征(SIRS)或败血症迹象进行每日随访,并将患者分为 SIRS 和非 SIRS 亚组,然后根据是否出现严重败血症将患者分为两组。随访患者的 CD64 和 MPO 样本,以评估其预后价值。39.58%的患者出现 SIRS,20.8%的患者出现严重败血症。病例的 CD64 和 MPO 明显高于对照组(分别为 p= 0.003 和 p <0.001),SIRs 和严重败血症患者的 CD64 分别为 1559.00± 367.09 pg/ml 和 1547.9 4± 436.14 pg/ml。此外,SIRS(113.58± 25.19 mU/ml)和严重败血症(111.70± 26.50 mU/ml)患者的 MPO 也明显升高。入院患者发生败血症后,CD64 和 MPO 明显升高。入院时 CD64 和 MPO 的 ROC 明显高于入院时的 CRP(分别为 p=0.123 和 p=0.014)。总之,外周血中的血浆 CD64 和 MPO 水平可被视为检测和随访小儿败血症的早期敏感标志物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Role of CD64 and myeloperoxidase as biomarkers for early diagnosis of sepsis in pediatric intensive care unit.

Globally, sepsis is the primary cause of death for children. While research conducted on adults has a significant impact on the diagnosis and treatment of sepsis in newborns and young children, there are significant factors that are pertinent to pediatrics as well. This prospective case-control study was conducted during the period from August 2020 to October 2022 after approval by the institutional ethical committee. The study included 48 critically ill children admitted at the Pediatric intensive care unit and 30 apparently healthy children as a control group. Laboratory investigations including complete blood picture, C-reactive protein (CRP), blood culture and sensitivity and plasma level of cluster of differentiation 64 (CD64) and myeloperoxidase (MPO) were investigated for all participants. A daily follow up for the signs of systemic inflammatory response syndrome (SIRS) or sepsis was done, and the patients were divided into SIRS and non-SIRS subgroups then patients were divided into two groups according to the presence of severe sepsis. A follow up CD64 and MPO sample were withdrawn from them to assess their prognostic value. SIRS was reported in 39.58 % of patients while severe sepsis was reported in 20.8%. CD64 and MPO were significantly higher in cases than controls (p= 0.003, p < 0.001, respectively) and, in patients with SIRs and severe sepsis CD64 was 1559.00± 367.09 pg/ml and 1547.9 4± 436.14 pg/ml, respectively. Also, MPO was significantly higher in patients with SIRS (113.58± 25.19 mU/ml) and severe sepsis (111.70± 26.50 mU/ml). CD64 and MPO significantly increased after development of sepsis in admitted patients. ROC was significantly higher for CD64 and MPO at admission than that for CRP at admission (p=0.123, p=0.014, respectively). In conclusion, plasma level of CD64 and MPO in peripheral blood can be considered an early sensitive marker for the detection and follow up of pediatric sepsis.

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CiteScore
1.20
自引率
0.00%
发文量
52
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