Oussalah Abderrahim, Callet Jonas, Manteaux Anne-Elisabeth, Thilly Nathalie, Jay Nicolas, Guéant Jean-Louis, Lozniewski Alain
Department of Molecular Medicine, Division of Biochemistry, Molecular Biology, and Nutrition, University Hospital of Nancy, Rue du Morvan, F-54511, Vandoeuvre-lès-Nancy, France.
Nutrition, Genetics, and Environmental Risk Exposure (NGERE, INSERM UMR_S 1256), Faculty of Medicine of Nancy, University of Lorraine, INSERM, 9, Avenue de la Forêt de Haye, F-54511, Vandoeuvre-lès-Nancy, France.
Biomark Res. 2023 Jan 17;11(1):4. doi: 10.1186/s40364-023-00450-3.
To assess the association between plasma procalcitonin concentration at hospital admission and the risk of 50-day in-hospital mortality among patients with community-acquired bloodstream infections.
We carried out a retrospective, observational cohort study with all consecutive patients with bacteriologically confirmed community-acquired bloodstream infections hospitalized between 2006 and 2012. We aimed to assess the association between plasma procalcitonin at admission and 50-day in-hospital mortality. Patients were included in the analysis if they had undergone a blood culture test within 48 hours of hospitalization with a concomitant procalcitonin assay (time < 12 hours between the two tests). Inclusion in the study began on the day of hospital admission, and each patient was followed until death, discharge from the hospital, or last known follow-up in the 50 days following hospital admission. The endpoint was the occurrence of all-cause in-hospital mortality during the 50 days following hospital admission.
During the 7-year study period, 1593 patients were admitted to one of the healthcare facilities of the University Hospital of Nancy from home or through the emergency department and had positive blood cultures and concomitant procalcitonin assays. Among the patients, 452 met the selection criteria and were analyzed. In ROC analysis, procalcitonin at baseline was significantly associated with 50-day in-hospital mortality, with an optimal threshold > 4.24 ng/mL. A baseline procalcitonin > 4.24 ng/mL was independently associated with an increased risk of in-hospital mortality (multivariable logistic regression: odds ratio, 2.58; 95% CI, 1.57-4.25; P = 0.0002; Cox proportional hazard regression: hazard ratio, 2.01; 95% CI, 1.30-3.11; P = 0.002). In sensitivity analyses, baseline procalcitonin quartiles were independently associated with 50-day in-hospital mortality (multivariable logistic regression: odds ratio, 1.47; 95% CI, 1.17-1.85; P = 0.001; Cox proportional hazard regression: hazard ratio, 1.31; 95% CI, 1.07-1.60; P = 0.008). The independent associations between baseline procalcitonin and the risk of 50-day in-hospital mortality were maintained after adjusting for C-reactive protein and sepsis status at admission.
Our data provide the first evidence of the usefulness of plasma procalcitonin at admission as a risk-stratifying biomarker for predicting 50-day in-hospital mortality among patients with community-acquired bloodstream infections.
评估社区获得性血流感染患者入院时血浆降钙素原浓度与50天内院内死亡风险之间的关联。
我们开展了一项回顾性观察队列研究,纳入2006年至2012年间所有连续住院且经细菌学确诊为社区获得性血流感染的患者。我们旨在评估入院时血浆降钙素原与50天内院内死亡之间的关联。如果患者在住院48小时内进行了血培养检测并同时进行了降钙素原检测(两次检测时间间隔<12小时),则纳入分析。研究纳入从入院当天开始,每位患者随访至死亡、出院或入院后50天内的最后一次已知随访。终点为入院后50天内全因院内死亡的发生情况。
在7年的研究期间,1593例患者从家中或通过急诊科入住南锡大学医院的医疗设施之一,血培养呈阳性且同时进行了降钙素原检测。其中,452例患者符合入选标准并进行了分析。在ROC分析中,基线降钙素原与50天内院内死亡显著相关,最佳阈值>4.24 ng/mL。基线降钙素原>4.24 ng/mL与院内死亡风险增加独立相关(多变量逻辑回归:比值比,2.58;95%CI,1.57 - 4.25;P = 0.0002;Cox比例风险回归:风险比,2.01;95%CI,1.30 - 3.11;P = 0.002)。在敏感性分析中,基线降钙素原四分位数与50天内院内死亡独立相关(多变量逻辑回归:比值比,1.47;95%CI,1.17 - 1.85;P = 0.001;Cox比例风险回归:风险比,1.31;95%CI,1.07 - 1.60;P = 0.008)。在调整入院时的C反应蛋白和脓毒症状态后,基线降钙素原与50天内院内死亡风险之间的独立关联仍然存在。
我们的数据首次证明了入院时血浆降钙素原作为预测社区获得性血流感染患者50天内院内死亡风险分层生物标志物的有用性。
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