Risk prediction with procalcitonin and clinical rules in community-acquired pneumonia

David T Huang; Lisa A Weissfeld; John A Kellum; Donald M Yealy; Lan Kong; Michael Martino; Derek C Angus; GenIMS Investigators

doi:10.1016/j.annemergmed.2008.01.003

Risk prediction with procalcitonin and clinical rules in community-acquired pneumonia

Ann Emerg Med. 2008 Jul;52(1):48-58.e2. doi: 10.1016/j.annemergmed.2008.01.003. Epub 2008 Mar 17.

Authors

David T Huang¹, Lisa A Weissfeld, John A Kellum, Donald M Yealy, Lan Kong, Michael Martino, Derek C Angus; GenIMS Investigators

Affiliation

¹ Clinical Research, Investigation, and Systems Modeling of Acute Illness Laboratory, Department of Critical Care Medicine, University of Pittsburgh, Pittsburgh, PA, USA.

Abstract

Study objective: The Pneumonia Severity Index and CURB-65 predict outcomes in community-acquired pneumonia but have limitations. Procalcitonin, a biomarker of bacterial infection, may provide prognostic information in community-acquired pneumonia. Our objective is to describe the pattern of procalcitonin in community-acquired pneumonia and determine whether procalcitonin provides prognostic information beyond the Pneumonia Severity Index and CURB-65.

Methods: We conducted a multicenter prospective cohort study in 28 community and teaching emergency departments. Patients presenting with a clinical and radiographic diagnosis of community-acquired pneumonia were enrolled. We stratified procalcitonin levels a priori into 4 tiers: I: less than 0.1; II: greater than 0.1 to less than 0.25; III: greater than 0.25 to less than 0.5; and IV: greater than 0.5 ng/mL. Primary outcome was 30-day mortality.

Results: One thousand six hundred fifty-one patients formed the study cohort. Procalcitonin levels were broadly spread across tiers: 32.8% (I), 21.6% (II), 10.2% (III), and 35.4% (IV). Used alone, procalcitonin had modest test characteristics: specificity (35%), sensitivity (92%), positive likelihood ratio (1.41), and negative likelihood ratio (0.22). Adding procalcitonin to the Pneumonia Severity Index in all subjects minimally improved performance. Adding procalcitonin to low-risk Pneumonia Severity Index subjects (classes I to III) provided no additional information. However, subjects in procalcitonin tier I had low 30-day mortality, regardless of clinical risk, including those in higher risk classes (1.5% versus 1.6% for those in Pneumonia Severity Index classes I to III versus classes IV/V). Among high-risk Pneumonia Severity Index subjects (classes IV/V), one quarter (126/546) were in procalcitonin tier I, and the negative likelihood ratio of procalcitonin tier I was 0.09. Procalcitonin tier I was also associated with lower burden of other adverse outcomes. Similar results were observed with CURB-65 stratification.

Conclusion: Selective use of procalcitonin as an adjunct to existing rules may offer additional prognostic information in high-risk patients.

Publication types

Multicenter Study

MeSH terms

Aged
Biomarkers / blood
Calcitonin / blood*
Calcitonin Gene-Related Peptide
Community-Acquired Infections / blood*
Community-Acquired Infections / mortality
Female
Humans
Likelihood Functions
Male
Pneumonia / blood*
Pneumonia / mortality
Prognosis
Prospective Studies
Protein Precursors / blood*
Risk Assessment
Sensitivity and Specificity
Severity of Illness Index
Survival Analysis

Substances

Biomarkers
CALCA protein, human
Protein Precursors
Calcitonin
Calcitonin Gene-Related Peptide

Abstract

Publication types

MeSH terms

Substances

Grants and funding