Abstract

Introduction: Approximately 3% of hospitalized patients with community-acquired bacterial pneumonia (CABP) develop healthcare-associated Clostridioides difficile infection (HCA-CDI). The validated Davis risk score (DRS) indicates that patients with a DRS ≥ 6 are at an increased risk of 30-day HCA-CDI. In the phase 3 OPTIC CABP study, 14% of CABP patients with DRS ≥ 6 who received moxifloxacin developed CDI vs. 0% for omadacycline. This study assessed the potential economic impact of substituting current guideline-concordant CABP inpatient treatments with omadacycline in hospitalized CABP patients with a DRS ≥ 6 across US hospitals. Methods: A deterministic healthcare-decision analytic model was developed. The model population was hospitalized adult CABP patients with a DRS ≥ 6 across US hospitals (100,000 patients). In the guideline-concordant arm, 14% of CABP patients with DRS ≥ 6 were assumed to develop an HCA-CDI, each costing USD 20,100. In the omadacycline arm, 5 days of therapy was calculated for the entire model population. Results: The use of omadacycline in place of guideline-concordant CABP inpatient treatments for CABP patients with DRS ≥ 6 was estimated to result in cost savings of USD 55.4 million annually across US hospitals. Conclusion: The findings of this simulated model suggest that prioritizing the use of omadacycline over current CABP treatments in hospitalized CABP with a DRS ≥ 6 may potentially reduce attributable HCA-CDI costs. The findings are not unique to omadacycline and could be applied to any antibiotic that confers a lower risk of HCA-CDI relative to current CABP inpatient treatments.

Highlights

  • 3% of hospitalized patients with community-acquired bacterial pneumonia (CABP) develop healthcare-associated Clostridioides difficile infection (HCA-CDI).The validated Davis risk score (DRS) indicates that patients with a DRS ≥ 6 are at an increased risk of 30-day HCA-CDI

  • The intent of this study was to assess the economic impact of prioritizing the use of omadacycline, over other guideline-concordant inpatient therapies [19], in hospitalized CABP patients at high risk for CDI [3]

  • It is well documented that the use of guideline-concordant antibiotics such as fluoroquinolones and the advanced generation cephalosporins are associated with increased CDI risks [1,2,3,4,5,6,7,16,19]

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Summary

Introduction

3% of hospitalized patients with community-acquired bacterial pneumonia (CABP) develop healthcare-associated Clostridioides difficile infection (HCA-CDI).The validated Davis risk score (DRS) indicates that patients with a DRS ≥ 6 are at an increased risk of 30-day HCA-CDI. Results: The use of omadacycline in place of guideline-concordant CABP inpatient treatments for CABP patients with DRS ≥ 6 was estimated to result in cost savings of USD 55.4 million annually across US hospitals. Conclusion: The findings of this simulated model suggest that prioritizing the use of omadacycline over current CABP treatments in hospitalized CABP with a DRS ≥ 6 may potentially reduce attributable HCA-CDI costs. Infections due to Clostridioides difficile (CDI), a common adverse effect associated with use of board-spectrum antibiotic therapy [1,2,3,4,5,6,7], is a leading cause of healthcare-associated infections Such infections cause an estimated 2.24 cases per 1000 hospital admissions per year [8]. Given that use of broad-spectrum antibiotics, in large part, drive healthcare-associated CDI (HCA-CDI) rates [1,2,3,4,5,6], there is need to proactively use validated CDI risk stratification tools such as the Davis risk score (DRS) [3] to minimize the use of high CDI risk antibiotics [16], such as fluoroquinolones and ceftriaxone, in high-CDI-risk patients as a primary HCA-CDI prevention measure

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