Literature DB >> 22726372

D-dimer levels in assessing severity and clinical outcome in patients with community-acquired pneumonia. A secondary analysis of a randomised clinical trial.

Dominic Snijders1, Margreet Schoorl, Marianne Schoorl, Piet C Bartels, Tjip S van der Werf, Wim G Boersma.   

Abstract

BACKGROUND: D-dimer levels are in several studies elevated in patients with CAP. In this study we assess the use of D-dimer levels and its association with severity assessment and clinical outcome in patients hospitalised with community-acquired pneumonia.
METHODS: In a subset of randomised trial patients with community-acquired pneumonia serial D-dimer levels was analysed. CURB-65 scores were calculated at admission.
RESULTS: A total of 147 patients were included. D-dimer levels at admission were higher in patients with severe CAP (2166 ± 1258 versus 1630 ± 1197 μg/l, p=0.03), with clinical failure at day 30 (2228 ± 1512 versus 1594 ± 1078 μg/l, p=0.02) and with early failure (2499 ± 1817 μg/l versus 1669 ± 1121 μg/l, p=0.01). Non-survivors had higher D-dimer levels (3025 ± 2105 versus 1680 ± 1128 μg/l, p=0.05). None of the 16 patients with D-dimer levels<500 μg/l died. In multivariate analysis D-dimer levels were not associated with clinical outcome. D-dimer levels have poor accuracy for predicting clinical outcome at day 30 (AUC 0.62, 95% CI 0.51-0.73) or 30 day mortality (AUC 0.71 (95% CI 0.51-0.91)). Addition of D-dimer levels to CURB-65 did not increase accuracy. No differences were observed in serial D-dimer levels between patients with clinical success or failure at day 30.
CONCLUSION: D-dimer levels are elevated in patients with CAP. Significantly higher D-dimer levels are found in patients with clinical failure and with severe CAP. D-dimer levels as single biomarker or as addition to the CURB-65 have no added value for predicting clinical outcome or mortality. D-dimer levels<500 μg/l may identify candidates at low risk for complications.
Copyright © 2011 European Federation of Internal Medicine. Published by Elsevier B.V. All rights reserved.

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Year:  2011        PMID: 22726372     DOI: 10.1016/j.ejim.2011.10.019

Source DB:  PubMed          Journal:  Eur J Intern Med        ISSN: 0953-6205            Impact factor:   4.487


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