| Literature DB >> 27258068 |
Christos A Grigoras1,2, Fainareti N Zervou1, Ioannis M Zacharioudakis1, Constantinos I Siettos2, Eleftherios Mylonakis1.
Abstract
Clostridium difficile infection is the most common hospital-acquired infection. Besides infected patients, carriers have emerged as a key player in C. difficile epidemiology. In this study, we evaluated the impact of identifying and isolating carriers upon hospital admission on the incidence of CDI incidence and hospital-acquired C. difficile colonization, as a single policy and as part of bundle approaches. We simulated C. difficile transmission using a stochastic mathematical approach, considering the contribution of carriers based on published literature. In the baseline scenario, CDI incidence was 6.18/1,000 admissions (95% CI, 5.72-6.65), simulating reported estimates from U.S. hospital discharges. The acquisition rate of C. difficile carriage was 9.72/1,000 admissions (95% CI, 9.15-10.31). Screening and isolation of colonized patients on admission to the hospital decreased CDI incidence to 4.99/1,000 admissions (95% CI, 4.59-5.42; relative reduction (RR) = 19.1%) and led to 36.2% reduction in the rate of hospital-acquired colonization. Simulating an antimicrobial stewardship program reduced CDI rate to 2.35/1,000 admissions (95% CI, 2.07-2.65). In sensitivity analysis, CDI incidence was less than 2.32/1,000 admissions (RR = 62.4%) in 95% of 1,000 simulations. The combined bundle, focusing on reducing C. difficile transmission from colonized patients and the individual risk of these patients to develop CDI, decreased significantly the incidence of both CDI and hospital-acquired colonization. Implementation of this bundle to current practice is expected to have an important impact in containing CDI.Entities:
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Year: 2016 PMID: 27258068 PMCID: PMC4892551 DOI: 10.1371/journal.pone.0156577
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Fig 1Schematic of the model describing the transmission dynamics of C. difficile.
Model Inputs.
C. difficile = Clostridium difficile, CDI = Clostridium difficile infection, PCR = polymerase-chain reaction, R = reference.
| Baseline Probabilities | Value (range) | Source |
|---|---|---|
| CDI Prevalence on Admission, U.S. ( | 0.003 | [ |
| CDI Incidence among U.S. Hospital Discharges | 8.2 per 1,000 discharges | [ |
| 0.10 (0.071–0.134) | [ | |
| Mean Length of Stay for Non-Infected Patients (days) (1/d) | 4.5 | [ |
| Mean Length of Stay Attributable to CDI (days) (1/di) | 2.9 | [ |
| Risk of Short-Term Colonized Patients to Develop CDI During Hospital Stay ( | 0.60 | [ |
| Mean Time for Short-Term Colonized Patients to Develop CDI (days) ( | 2 | [ |
| Percentage of CDIs coming from colonized on admission patients | 0.341 (0.195–0.505) | [ |
| Relative Reduction of CDI Incidence after Implementation of an Antimicrobial Stewardship Program ( | 0.52 (0.38–0.62) | [ |
| Sensitivity of PCR compared to toxinogenic culture ( | 0.92 (0.91–0.94) | [ |
| Compliance with contact precautions ( | 0.772 (0.632–1.0) | [ |
| Prevalence of contact precautions to admitted patients for MRSA or VRE colonization and/ or infection ( | 0.047 (0.045–0.049) | [ |
Summary estimates of CDI incidence per 1,000 admissions and rate of newly colonized with C. difficile patients per 1,000 admissions.
C. difficile = Clostridium difficile, CDI = Clostridium difficile infection, CIs = confidence intervals, R = reference.
| Baseline | 6.18 (5.72–6.65) | - |
| Screening and Contact Precautions | 4.99 (4.59–5.42) | 19.1 |
| Screening, Contact Precautions and Antimicrobial Stewardship | 2.35 (2.08–2.65) | 61.88 |
| Baseline | 9.72 (9.15–10.31) | - |
| Screening and Contact Precautions | 6.21 (5.75–8.5) | 36.22 |
| Screening, Contact Precautions and Antimicrobial Stewardship | 4.22 (3.85–4.61) | 56.6 |
Fig 2Probabilistic sensitivity analysis.
Histogram of the incidence rate in 1,000 simulations. In 95% of simulations the incidence rate is below 2.32 per 1,000 admissions (dashed line), corresponding to a 62.4% reduction of the baseline CDI rate.