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Mortality Risk in Pediatric Sepsis Based on C-reactive Protein and Ferritin Levels

医学 败血症 血清铁蛋白 铁蛋白 C反应蛋白 重症监护医学 内科学 儿科 炎症
作者
Christopher M. Horvat,Anthony Fabio,Daniel S. Nagin,Russell Banks,Yidi Qin,Hyun Jung Park,Kate F. Kernan,Scott Canna,Robert A. Berg,David Wessel,Murray M. Pollack,Kathleen L. Meert,Mark W. Hall,Christopher J. L. Newth,John C. Lin,Allan Doctor,Thomas P. Shanley,Tim Cornell,Rick Harrison,Athena F. Zuppa,Ron Reeder,Katherine Sward,Richard Holubkov,Daniel A. Notterman,J. Michael Dean,Joseph A. Carcillo
出处
期刊:Pediatric Critical Care Medicine [Ovid Technologies (Wolters Kluwer)]
卷期号:23 (12): 968-979 被引量:19
标识
DOI:10.1097/pcc.0000000000003074
摘要

OBJECTIVES: Interest in using bedside C-reactive protein (CRP) and ferritin levels to identify patients with hyperinflammatory sepsis who might benefit from anti-inflammatory therapies has piqued with the COVID-19 pandemic experience. Our first objective was to identify patterns in CRP and ferritin trajectory among critically ill pediatric sepsis patients. We then examined the association between these different groups of patients in their inflammatory cytokine responses, systemic inflammation, and mortality risks. DATA SOURCES: A prospective, observational cohort study. STUDY SELECTION: Children with sepsis and organ failure in nine pediatric intensive care units in the United States. DATA EXTRACTION: Two hundred and fifty-five children were enrolled. Five distinct clinical multi-trajectory groups were identified. Plasma CRP (mg/dL), ferritin (ng/mL), and 31 cytokine levels were measured at two timepoints during sepsis (median Day 2 and Day 5). Group-based multi-trajectory models (GBMTM) identified groups of children with distinct patterns of CRP and ferritin. DATA SYNTHESIS: Group 1 had normal CRP and ferritin levels ( n = 8; 0% mortality); Group 2 had high CRP levels that became normal, with normal ferritin levels throughout ( n = 80; 5% mortality); Group 3 had high ferritin levels alone ( n = 16; 6% mortality); Group 4 had very high CRP levels, and high ferritin levels ( n = 121; 11% mortality); and Group 5 had very high CRP and very high ferritin levels ( n = 30; 40% mortality). Cytokine responses differed across the five groups, with ferritin levels correlated with macrophage inflammatory protein 1α levels and CRP levels reflective of many cytokines. CONCLUSIONS: Bedside CRP and ferritin levels can be used together to distinguish groups of children with sepsis who have different systemic inflammation cytokine responses and mortality risks. These data suggest future potential value in personalized clinical trials with specific targets for anti-inflammatory therapies.
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