Predicting the risk of documented ventilator-associated pneumonia for benchmarking: construction and validation of a score

Jean-Ralph Zahar; Moliere Nguile-Makao; Adrien Français; Carole Schwebel; Maité Garrouste-Orgeas; Dany Goldgran-Toledano; Elie Azoulay; Marie Thuong; Samir Jamali; Yves Cohen; Arnaud de Lassence; Jean-François Timsit

doi:10.1097/CCM.0b013e3181a38109

Predicting the risk of documented ventilator-associated pneumonia for benchmarking: construction and validation of a score

Crit Care Med. 2009 Sep;37(9):2545-51. doi: 10.1097/CCM.0b013e3181a38109.

Authors

Jean-Ralph Zahar¹, Moliere Nguile-Makao, Adrien Français, Carole Schwebel, Maité Garrouste-Orgeas, Dany Goldgran-Toledano, Elie Azoulay, Marie Thuong, Samir Jamali, Yves Cohen, Arnaud de Lassence, Jean-François Timsit

Affiliation

¹ Microbiology and Infection Control Unit (J-RZ), Necker Teaching Hospital, Paris France.

PMID: 19623046
DOI: 10.1097/CCM.0b013e3181a38109

Abstract

Objectives: : To build and validate a ventilator-associated pneumonia risk score for benchmarking. The rate of ventilator-associated pneumonia varies widely with case-mix, a fact that has limited its use for measuring intensive care unit performance.

Methods: : We studied 1856 patients in the OUTCOMEREA database treated at intensive care unit admission by endotracheal intubation followed by mechanical ventilation for >48 hrs; they were allocated randomly to a training data set (n = 1233) or a validation data set (n = 623). Multivariate logistic regression was used. Calibration of the final model was assessed in both data sets, using the Hosmer-Lemeshow chi-square test and receiver operating characteristic curves.

Measurements and main results: : Independent risk factors for ventilator-associated pneumonia were male gender (odds ratio = 1.97, 95% confidence interval = 1.32-2.95); SOFA at intensive care unit admission (<3 [reference value], 3-4 [2.57, 1.39-4.77], 5-8 [7.37, 4.24-12.81], >8 [5.81 (3.2-10.52)], no use within 48 hrs after intensive care unit admission of parenteral nutrition (2.29, 1.52-3.45), no broad-spectrum antimicrobials (2.11, 1.46-3.06); and mechanical ventilation duration (<5 days (); 5-7 days (17.55, 4.01-76.85); 7-15 days (53.01, 12.74-220.56); >15 days (225.6, 54.3-936.7). Tests in the training set showed good calibration and good discrimination (area under the curve-receiver operating characteristic curve = 0.881), and both criteria remained good in the validation set (area under the curve-receiver operating characteristic curve = 0.848) and good calibration (Hosmer-Lemeshow chi-square = 9.98, p = .5). Observed ventilator-associated pneumonia rates varied across intensive care units from 9.7 to 26.1 of 1000 mechanical ventilation days but the ratio of observed over theoretical ventilator-associated pneumonia rates was >1 in only two intensive care units.

Conclusions: : The ventilator-associated pneumonia rate may be useful for benchmarking provided the ratio of observed over theoretical rates is used. External validation of our prediction score is needed.

Publication types

Randomized Controlled Trial
Research Support, Non-U.S. Gov't
Validation Study

MeSH terms

Aged
Benchmarking*
Female
Humans
Male
Middle Aged
Pneumonia, Ventilator-Associated / epidemiology*
Prognosis
Risk Assessment
Risk Factors