Circulating galectin-3 in infections and non-infectious inflammatory diseases

被引:0
|
作者
J. ten Oever
E. J. Giamarellos-Bourboulis
F. L. van de Veerdonk
F. F. Stelma
A. Simon
M. Janssen
M. Johnson
A. Pachot
B.-J. Kullberg
L. A. B. Joosten
M. G. Netea
机构
[1] Radboud University Nijmegen Medical Center,Department of Medicine
[2] Radboud University Nijmegen Medical Center,Department of Medical Microbiology
[3] Nijmegen Institute for Infection,4th Department of Internal Medicine
[4] Inflammation & Immunity (N4i),Department of Rheumatology
[5] University of Athens,Biomarker Department
[6] Medical School,Department of Internal Medicine (463)
[7] Rijnstate Hospital,undefined
[8] Duke University Medical Center,undefined
[9] bioMérieux,undefined
[10] Radboud University Nijmegen Medical Center,undefined
关键词
Gout; Invasive Candidiasis; Bacterial Sepsis; Autoinflammatory Syndrome; Candida Sepsis;
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学科分类号
摘要
Recent studies point to a dual role for galectin-3 as both a circulating damage-associated molecular pattern and a cell membrane-associated pattern recognition receptor. The aim of this study was to assess the potential of circulating galectin-3 for discriminating between infections and non-infectious inflammatory disorders on the one hand, and between fungal and bacterial infections on the other. Galectin-3 and C-reactive protein (CRP) were measured in the plasma of 127 patients with either non-infectious inflammatory disorders (gout, autoinflammatory syndrome or pancreatitis) or an infection (viral lower respiratory tract infection, bacterial sepsis or candidaemia). Circulating galectin-3 concentrations were increased in patients with infections when compared with healthy volunteers or patients with non-infectious inflammatory diseases. At cut-off values with a specificity of 95 %, the sensitivity of galectin-3 (>20.6 ng/ml) to discriminate between an infection and non-infectious inflammation was higher than that of CRP (>156 mg/l): 43 % [95 % confidence interval (CI) 33–53 %] versus 27 % (95 % CI 19–37 %), p = 0.03. After exclusion of patients with CRP <156 mg/l, galectin-3 concentration >20.6 ng/ml could identify 41 % (95 % CI 29–53 %) of the patients with an infection at the cost of one false-positive with non-infectious inflammation. Using this sequential approach, 57 % of the patients with an infection could be selected. Galectin-3 concentrations were similar in patients with bacterial and Candida sepsis, while being lower in viral respiratory infections. Although galectin-3 does not discriminate between bacterial and Candida sepsis, the sequential use of CRP and galectin-3 in distinguishing infectious diseases from non-infectious inflammation may be superior to CRP alone.
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页码:1605 / 1610
页数:5
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