Prohormones for Prediction of Adverse Medical Outcome in Community-acquired Pneumonia and Lower Respiratory Tract Infections

Overview

Journal Crit Care

Specialty Critical Care

Date 2010 Jun 10

PMID 20529344

Citations 47

Authors

Philipp Schuetz

Marcel Wolbers

Mirjam Christ-Crain

Robert Thomann

Claudine Falconnier

Isabelle Widmer

Stefanie Neidert

Thomas Fricker

Claudine Blum

Ursula Schild

Nils G Morgenthaler

Ronald Schoenenberger

Christoph Henzen

Thomas Bregenzer

Claus Hoess

Martin Krause

Heiner C Bucher

Werner Zimmerli

Beat Mueller

Affiliations

Soon will be listed here.

Abstract

Introduction: Measurement of prohormones representing different pathophysiological pathways could enhance risk stratification in patients with community-acquired pneumonia (CAP) and other lower respiratory tract infections (LRTI).

Methods: We assessed clinical parameters and five biomarkers, the precursor levels of adrenomedullin (ADM), endothelin-1 (ET1), atrial-natriuretic peptide (ANP), anti-diuretic hormone (copeptin), and procalcitonin in patients with LRTI and CAP enrolled in the multicenter ProHOSP study. We compared the prognostic accuracy of these biomarkers with the pneumonia severity index (PSI) and CURB65 (Confusion, Urea, Respiratory rate, Blood pressure, Age 65) score to predict serious complications defined as death, ICU admission and disease-specific complications using receiver operating curves (ROC) and reclassification methods.

Results: During the 30 days of follow-up, 134 serious complications occurred in 925 (14.5%) patients with CAP. Both PSI and CURB65 overestimated the observed mortality (X2 goodness of fit test: P = 0.003 and 0.01). ProADM or proET1 alone had stronger discriminatory powers than the PSI or CURB65 score or any of either score components to predict serious complications. Adding proADM alone (or all five biomarkers jointly) to the PSI and CURB65 scores, significantly increased the area under the curve (AUC) for PSI from 0.69 to 0.75, and for CURB65 from 0.66 to 0.73 (P < 0.001, for both scores). Reclassification methods also established highly significant improvement (P < 0.001) for models with biomarkers if clinical covariates were more flexibly adjusted for. The developed prediction models with biomarkers extrapolated well if evaluated in 434 patients with non-CAP LRTIs.

Conclusions: Five biomarkers from distinct biologic pathways were strong and specific predictors for short-term adverse outcome and improved clinical risk scores in CAP and non-pneumonic LRTI. Intervention studies are warranted to show whether an improved risk prognostication with biomarkers translates into a better clinical management and superior allocation of health care resources.

Trial Registration: NCT00350987.

Citing Articles

Mid-Regional Proadrenomedullin Levels in Primary Immunodeficiencies Complicated with Pulmonary Manifestations.

Azarsiz E, Karaca N, Kutukculer N Indian J Clin Biochem. 2023; 38(4):475-484.

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A Nomogram for Early Diagnosis of Community-Acquired Pneumonia Based on Bronchoalveolar Lavage Fluid Metabolomics.

Chen S, Su M, Lei W, Wu Z, Wu S, Liu J Infect Drug Resist. 2023; 16:1237-1248.

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Development and validation of tools for predicting the risk of death and ICU admission of non-HIV-infected patients with pneumonia.

Jin F, Liang H, Chen W, Xie J, Wang H Front Public Health. 2022; 10:972311.

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Mid-regional pro-adrenomedullin as a predictor of in-hospital mortality in adult patients with COVID-19: a single-centre prospective study.

Popov D, Borovkova U, Rybka M, Ramnyonok T, Golukhova E Anaesthesiol Intensive Ther. 2022; 54(3):242-246.

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Association of Serum Albumin and Copeptin with Early Clinical Deterioration and Instability in Community-Acquired Pneumonia.

Parthasarathi A, Padashetti V, Padukudru S, Chaya S, Siddaiah J, Anand M Adv Respir Med. 2022; 90(4):323-337.

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