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The Associations of Serum S100A9 with the Severity and Prognosis In Patients With Community-Acquired Pneumonia: A Retrospective Cohort Study
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Abstract
Background: Previous studies found that S100A9 may involve in the pathophysiology of community-acquired pneumonia (CAP). However, the role of S100A9 in the CAP was unclear. The goal was to explore the correlations of serum S100A9 with the severity and prognosis of CAP patients based on a retrospective cohort study.Methods: A total of 220 CAP patients and 110 control subjects were recruited. Demographic and clinical data were extracted. Serum S100A9 and inflammatory cytokines were measured.Results: Serum S100A9 was elevated in CAP patients on admission. Furthermore, serum S100A9 was gradually elevated parallelly with CAP severity scores. Inflammatory cytokines were increased and blood routine parameters were changed in CAP patients compared with control subjects. Correlation analysis found that serum S100A9 was positively associated with CAP severity scores, blood routine parameters (WBC, NLR and MON) and inflammatory cytokines. Furtherly, logistical regression demonstrated that there were positive associations between serum S100A9 and CAP severity scores. Besides, the prognosis of CAP was tracked. Serum higher S100A9 on the early stage was positively correlated with the death of risk and hospital stay among CAP patients. Conclusion: Serum S100A9 is positively correlated with the severity of CAP. On admission, serum higher S100A9 elevates the risk of death and hospital stay in CAP patients, suggesting that S100A9 may exert a certain function in the pathophysiology of CAP and regard as a serum diagnostic and managing biomarker for CAP.
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Title: The Associations of Serum S100A9 with the Severity and Prognosis In Patients With Community-Acquired Pneumonia: A Retrospective Cohort Study
Description:
Abstract
Background: Previous studies found that S100A9 may involve in the pathophysiology of community-acquired pneumonia (CAP).
However, the role of S100A9 in the CAP was unclear.
The goal was to explore the correlations of serum S100A9 with the severity and prognosis of CAP patients based on a retrospective cohort study.
Methods: A total of 220 CAP patients and 110 control subjects were recruited.
Demographic and clinical data were extracted.
Serum S100A9 and inflammatory cytokines were measured.
Results: Serum S100A9 was elevated in CAP patients on admission.
Furthermore, serum S100A9 was gradually elevated parallelly with CAP severity scores.
Inflammatory cytokines were increased and blood routine parameters were changed in CAP patients compared with control subjects.
Correlation analysis found that serum S100A9 was positively associated with CAP severity scores, blood routine parameters (WBC, NLR and MON) and inflammatory cytokines.
Furtherly, logistical regression demonstrated that there were positive associations between serum S100A9 and CAP severity scores.
Besides, the prognosis of CAP was tracked.
Serum higher S100A9 on the early stage was positively correlated with the death of risk and hospital stay among CAP patients.
Conclusion: Serum S100A9 is positively correlated with the severity of CAP.
On admission, serum higher S100A9 elevates the risk of death and hospital stay in CAP patients, suggesting that S100A9 may exert a certain function in the pathophysiology of CAP and regard as a serum diagnostic and managing biomarker for CAP.
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