Elevated progranulin as a novel biomarker to predict poor prognosis in community-acquired pneumonia

•This prospective study assessed progranuin (PGRN) as a prognostic indicator.•Admission PGRN levels were elevated in community-acquired pneumonia (CAP) patients.•PGRN levels were not affected by different etiologies of CAP.•Higher PGRN levels were associated with higher odds of poor prognosis in CAP...

Full description

Saved in:
Bibliographic Details
Published in:The Journal of infection 2020-02, Vol.80 (2), p.167-173
Main Authors: Luo, Qiongzhen, He, Xinwei, Zheng, Yali, Ning, Pu, Xu, Yu, Yang, Donghong, Shang, Ying, Gao, Zhancheng
Format: Article
Language:English
Subjects:
Biomarkers
Community-Acquired Infections - diagnosis
Community-acquired pneumonia
Etiology
Humans
Odds ratio
Pneumonia
Prognosis
Progranulin
Progranulins
Prospective Studies
Severity of Illness Index
Citations: Items that this one cites
Items that cite this one
Online Access:Get full text
Tags: Add Tag
No Tags, Be the first to tag this record!
Description
Summary:•This prospective study assessed progranuin (PGRN) as a prognostic indicator.•Admission PGRN levels were elevated in community-acquired pneumonia (CAP) patients.•PGRN levels were not affected by different etiologies of CAP.•Higher PGRN levels were associated with higher odds of poor prognosis in CAP.•PGRN can improve the prognostic power of CURB-65 or PSI. Prognostic biomarkers help triage initial patients and inform targeted therapy selection. Here, we explored the role of progranulin (PGRN)—implicated in processes ranging from inflammation to neurodegeneration—in patients with community-acquired pneumonia (CAP). A prospective observational cohort study was conducted during 2017. Patients who required invasive mechanical ventilation and/or had septic shock and were discharged from the hospital were cohort II. Those who died at the hospital were cohort III. Remaining patients discharged from the hospital were cohort I. The primary endpoint was that patients progressed to served as cohort II; the secondary endpoint was that patients progressed to served as cohort III. Serum PGRN levels were detected by ELISA. A total of 280 patients constituted the study cohort. 194 (69.3%) were categorized into cohort I, 61 (21.8%) were categorized into cohort II, and 25 (8.9%) were categorized into cohort III. Serum PGRN levels were increased in CAP patients, independently of etiology. Adjusting for clinical parameters, the odds ratios (95%CI) of cohort III and combined cohort II–III were 34.968 (3.743–326.692) and 3.741 (1.496–9.351), respectively, comparing lowest-to-highest quartile PGRN levels. PGRN exhibited high accuracy in predicting 30-day mortality, with AUC 0.862. PGRN combined with CURB-65 or PSI significantly improved prediction performance. Cox proportional regression analysis showed PGRN was an independent predictor for 30-day mortality risk. Cox survival curves confirmed PGRN ≥89.51 ng/mL had a significantly higher mortality rate than PGRN
ISSN:0163-4453
1532-2742
DOI:10.1016/j.jinf.2019.12.004