SEPSIGN: early identification of sepsis signs in emergency department

被引:0
作者
Lafon, Thomas [1 ,2 ]
Cazalis, Marie-Angelique [3 ]
Hart, Kimberly W. [4 ]
Hennessy, Cassandra [4 ]
Tazarourte, Karim [5 ,6 ]
Self, Wesley H. [7 ,8 ]
Akhavan, Arvin Radfar [9 ]
Laribi, Said [10 ]
Viglino, Damien [11 ,12 ]
Douplat, Marion [13 ]
Ginde, Adit A. [14 ]
Tolou, Sophie [15 ]
Mahler, Simon A. [16 ,17 ,18 ]
Le Borgne, Pierrick [19 ,20 ]
Claessens, Yann-Erick [21 ]
Yordanov, Youri [22 ]
Le Bastard, Quentin [23 ]
Pancher, Agathe [24 ]
Ducharme, Jim [25 ]
Lindsell, Christopher J. [4 ]
Shapiro, Nathan I. [26 ]
机构
[1] Dupuytren Univ Hosp, Emergency Dept, 2 Ave Martin Luther King, F-87042 Limoges, France
[2] Dupuytren Univ Hosp, Inserm CIC 1435, 2 Ave Martin Luther King, F-87042 Limoges, France
[3] BioMerieux SA, Med Diagnost Discovery Dept MD3, Marcy Letoile, France
[4] Vanderbilt Univ, Med Ctr, Dept Biostat, Nashville, TN USA
[5] Univ Lyon 1, Ctr Hosp Univ Edouard Herriot, Emergency Dept, SAMU 69,Hosp Civils Lyon, Lyon, France
[6] Univ Lyon 1, Ctr Hosp Univ Edouard Herriot, INSERM 1290, RESHAPE, Lyon, France
[7] Vanderbilt Univ, Dept Emergency Med, Med Ctr, Nashville, TN USA
[8] Vanderbilt Univ, Vanderbilt Inst Clin & Translat Res, Med Ctr, Nashville, TN USA
[9] Univ Washington, Dept Emergency Med, Seattle, WA USA
[10] CHU Tours, Emergency Dept, Tours, France
[11] Ctr Hosp Univ Grenoble Alpes, Emergency Dept, Grenoble, France
[12] Ctr Hosp Univ Grenoble Alpes, HP2 Lab, INSERM, U1800, Grenoble, France
[13] Ctr Hosp Univ Lyon Sud, Emergency Dept, Hosp Civils Lyon, Pierre Benite, France
[14] Univ Colorado, Sch Med, Dept Emergency Med, Aurora, CO USA
[15] Montauban Hosp, Emergency Dept, Montauban, France
[16] Wake Forest Univ, Dept Emergency Med, Sch Med, Winston Salem, NC USA
[17] Wake Forest Univ, Dept Epidemiol & Prevent, Sch Med, Winston Salem, NC USA
[18] Wake Forest Univ, Dept Implementat Sci, Sch Med, Winston Salem, NC USA
[19] Univ Strasbourg, Hop Univ Strasbourg, Emergency Dept, Strasbourg, France
[20] Univ Strasbourg, Hop Univ Strasbourg, INSERM UMR 1260, Regenerat NanoMed,Fed Med Translat, Strasbourg, France
[21] Princesse Grace Hosp Ctr, Dept Emergency Med, Ave Pasteur, Monte Carlo, Monaco
[22] Sorbonne Univ, Hop St Antoine, AP HP,INSERM,UMR S 1136, Serv Accueil Urgences,Inst Pierre Louis Epidemiol, Paris, France
[23] Ctr Hosp Univ, Emergency Dept, Nantes, France
[24] Henri Mondor Hosp, Emergency Dept, Aurillac, France
[25] McMaster Univ, Dept Med, Hamilton, ON, Canada
[26] Beth Israel Deaconess Med Ctr, Dept Emergency Med, Boston, MA USA
关键词
Sepsis; Biomarkers; Triage; PLASMINOGEN-ACTIVATOR RECEPTOR; SEPTIC SHOCK; ANGIOPOIETIN-2; BIOMARKERS; PROCALCITONIN; DEFINITIONS; MECHANISMS; INFECTION; JUDGMENT;
D O I
10.1007/s11739-024-03802-5
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Because 20-30% of patients with sepsis deteriorate to critical illness, biomarkers that provide accurate early prognosis may identify which patients need more intensive treatment versus safe early discharge. The objective was to test the performance of sVEGFR2, suPAR and PCT, alone or combined with clinical signs and symptoms, for the prediction of clinical deterioration. This prospective observational study enrolled patients with suspected infection who met SIRS criteria without organ dysfunction (delta SOFA <2 from baseline) from 16 emergency departments. The primary endpoint was clinical deterioration (increased SOFA score >= 2 points, new or increased organ support, or death) within 72 hours of enrollment. Diagnosis and classification of infection status were adjudicated. 724 patients were enrolled, (54% men, median age 55 [38-70] y-o). Infection origin was abdominopelvic (21%), skin and soft tissues (17%), urinary (16%) and pulmonary (15%). 176 (24%) patients deteriorated, with a 28-day mortality of 1.4%. They had lower sVEGFR2 level (6.17 [5.00-7.40] vs 6.52 [5.40-7.84], p=0.024), higher circulating suPAR (5.25 [3.86-7.50] vs 4.18 [3.16-5.68], p<0.001) and higher PCT level (0.32 [0.08-1.80] vs 0.18 [0.05-0.98], p=0.004). suPAR demonstrated superior performance (AUC=0.65 [0.60-0.70]), compared to other biomarkers (PCT, AUC=0.57 [0.52-0.62] and sVEGFR2, AUC=0.58 [0.53-0.64]). Maximum accuracy was achieved from the combination of clinical information, sVEGFR2 and suPAR, yielding an AUC of 0.74 [0.69-0.78] and NPV 0.90 [0.88-0.94]. sVEGFR2 and suPAR were insufficiently accurate to rule out clinical deterioration. Panels of biomarkers will likely be needed to capture the heterogeneous mechanistic pathways involved in sepsis-related organ failure.
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页数:13
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