Identification of population at risk for future Clostridium difficile infection following hospital discharge to be targeted for vaccine trials. - PubMed - NCBI

Identification of population at risk for future Clostridium difficile infection following hospital discharge to be targeted for vaccine trials. - PubMed - NCBI

Vaccine. 2015 Oct 5. pii: S0264-410X(15)01354-7. doi: 10.1016/j.vaccine.2015.09.078. [Epub ahead of print]

Identification of population at risk for future Clostridium difficile infection following hospital discharge to be targeted for vaccine trials.

Baggs J1, Yousey-Hindes K2, Ashley ED3, Meek J2, Dumyati G3, Cohen J4, Wise M5, Clifford McDonald L5, Lessa FC5.

Author information

Abstract

BACKGROUND:

Efforts to develop a Clostridium difficile vaccine are underway; identification of patients at risk for C. difficile infection (CDI) is critical to inform vaccine trials. We identified groups at high risk of CDI≥28 days after hospital discharge.

METHODS:

Hospital discharge data and pharmacy data from two large academic centers, in New York and Connecticut, were linked to active population-based CDI surveillance data from the Emerging Infections Program (EIP). Adult residents of the EIP surveillance area were included if they had an inpatient stay at a study hospital without prior history of CDI. The primary outcome was CDI by either toxin or molecular assay ≥28 days after an index hospitalization. Important predictors of CDI≥28 days post discharge were initially identified through a Cox proportional hazards model (stepwise backward selection) using a derivation cohort; final model parameters were used to develop a risk score evaluated in the validation cohort.

RESULTS:

Of the 35,186 index hospitalizations, 288 (0.82%) had CDI≥28 days post discharge. After parameter selection, age, number of hospitalizations in the prior 90 days, admission diagnosis, and the use of 3rd/4th generation cephalosporin, clindamycin or fluoroquinolone antibiotic classes remained in the model. Using the validation cohort, the risk score was predictive (p<0.001) with a c-score of 0.75. Based on the distribution of scores in the derivation cohort, we divided the patients into low and high risk groups. In the high risk group, 1.6% experienced CDI≥28 days post discharge compared to 0.3% among our low risk group.

CONCLUSIONS:

Our study identified specific parameters for a risk score that can be applied at discharge to identify a patient population whose risk of CDI≥28 days following an acute care hospitalization was 5 times greater than other patients.

Copyright © 2015. Published by Elsevier Ltd.

KEYWORDS:

Administrative data; Anti-bacterial agents; Clostridium difficile infection; Health care-associated infections; Vaccines

PMID:

 

26450660

 

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