Bedside Risk Score Can Help Discriminate the Risk for MRSA Versus Other Pathogens
Methicillin-resistant Staphylococcus aureus (MRSA) is a frequent cause of complicated skin and skin structure infections (cSSSI). Patients with MRSA require different empiric treatment that those with non-MRSA infections, yet no accurate tools exist to aid in stratifying the risk for a MRSA cSSSI. Zilberberg, et al. sought to develop a simple bedside decision rule to tailor empiric coverage more accurately.
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The researchers conducted a large multicenter (N=62 hospitals) retrospective cohort study in a U.S.-based database between April 2005 and March 2009. All adult initial admissions with ICD-9-CM codes specific to cSSSI were included. Patients admitted with MRSA vs. non-MRSA were compared with regard to baseline demographic, clinical and hospital characteristics. We developed and validated a model to predict the risk of MRSA, and compared its performance via sensitivity, specificity and other classification statistics to the healthcare-associated (HCA) infection risk factors.
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Of the 7,183 patients with cSSSI, 2,387 (33.2 percent) had MRSA. Factors discriminating MRSA from non-MRSA were age, African-American race, no evidence of diabetes mellitus, cancer or renal dysfunction, and prior history of cardiac dysrhythmia. The score ranging from 0 to 8 points exhibited a consistent dose-response relationship. A MRSA score of 5 or higher was superior to the HCA classification in all characteristics, while that of 4 or higher was superior on all metrics except specificity.
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The researchers say that MRSA is present in one-third of all hospitalized cSSSI. They conclude that a simple bedside risk score can help discriminate the risk for MRSA versus other pathogens with improved accuracy compared to the HCA definition. Their research was published in
Reference: Zilberberg MD, et al. Development and validation of a bedside risk score for MRSA among patients hospitalized with complicated skin and skin structure infections. BMC Infectious Diseases 2012, 12:154 doi:10.1186/1471-2334-12-154
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