唾液 C 反应蛋白和平均血小板体积可作为晚期新生儿肺炎的诊断指标

Wafaa Ahmed Metwali‎, Abdelrahman Mohamed Elmashad, Sahar Mohey Eldin Hazzaa, Mohammed Al-Beltagi, Mohamed Basiony Hamza‎
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引用次数: 0

摘要

背景新生儿败血症对新生儿构成严重威胁,是新生儿死亡的主要原因之一,尤其是出生后 72 小时后出现的晚发性败血症更令人担忧。肺炎是一种常见的败血症表现,尤其是在新生儿期肺部防御功能受损时,肺炎构成了重大风险。肺炎的准确诊断对于及时有效的干预措施至关重要。唾液作为一种微创诊断介质,在评估感染(尤其是婴儿感染)方面大有可为。目的 研究血清 C 反应蛋白(CRP)、唾液 CRP(sCRP)和平均血小板体积(MPV)作为晚发型新生儿肺炎(LONP)诊断标志物的潜力。方法 对 80 名足月新生儿进行了系统检查,考虑了人体测量、临床表现、放射学检查结果以及包括血清 CRP、sCRP 和 MPV 在内的重要生物标志物。结果 研究显示,患有 LONP 的新生儿与健康对照组之间在血清 CRP 水平、MPV 和血清 CRP/MPV 比值方面存在显著差异。MPV 具有很强的判别能力[曲线下面积 (AUC) = 0.87],在临界值大于 8.8 时具有很高的灵敏度和特异性。此外,还发现了血清 CRP、sCRP 和 MPV 之间的相关性。值得注意的是,sCRP 对血清 CRP 水平具有极高的预测价值(AUC = 0.89),突出了其作为诊断工具的潜力。结论 本研究强调了唾液和血清生物标志物(尤其是 MPV 和 CRP)在识别和预测新生儿 LONP 方面的诊断前景。这些研究结果主张进一步开展研究,在更大的新生儿群体中验证它们的临床实用性。
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Salivary C-reactive protein and mean platelet volume as possible diagnostic markers for late-onset neonatal pneumonia
BACKGROUND Neonatal sepsis, a formidable threat to newborns, is a leading cause of neonatal mortality, with late-onset sepsis manifesting after 72 hours post-birth being particularly concerning. Pneumonia, a prevalent sepsis presentation, poses a significant risk, especially during the neonatal phase when lung defenses are compromised. Accurate diagnosis of pneumonia is imperative for timely and effective interventions. Saliva, a minimally invasive diagnostic medium, holds great promise for evaluating infections, especially in infants. AIM To investigate the potential of serum C-reactive protein (CRP), salivary CRP (sCRP), and mean platelet volume (MPV) as diagnostic markers for late-onset neonatal pneumonia (LONP). METHODS Eighty full-term neonates were systematically examined, considering anthropometric measurements, clinical manifestations, radiology findings, and essential biomarkers, including serum CRP, sCRP, and MPV. RESULTS The study reveals noteworthy distinctions in serum CRP levels, MPV, and the serum CRP/MPV ratio between neonates with LONP and healthy controls. MPV exhibited a robust discriminatory ability [area under the curve (AUC) = 0.87] with high sensitivity and specificity at a cutoff value of > 8.8. Correlations between serum CRP, sCRP, and MPV were also identified. Notably, sCRP demonstrated excellent predictive value for serum CRP levels (AUC = 0.89), underscoring its potential as a diagnostic tool. CONCLUSION This study underscores the diagnostic promise of salivary and serum biomarkers, specifically MPV and CRP, in identifying and predicting LONP among neonates. These findings advocate for further research to validate their clinical utility in larger neonatal cohorts.
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