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Original Research

Species-based comparison of disease severity and risk factors for disseminated Candida infections in pediatric patients

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Pages 59-70 | Published online: 18 Apr 2016
 

Abstract

Background

Pediatric Candida infections are associated with worse clinical outcomes and increased costs. Yet, it is not definitively known if particular species are associated with more severe illness. Differential risk factor exposures among the species group may also exist. We aimed to determine whether certain Candida species are more strongly associated with worse outcomes, and whether certain risk factors more strongly predispose patients to infection with certain species.

Methods

Microbiology lab records from patients seen from 2003 to 2010 at an urban children’s hospital were reviewed for invasive or disseminated Candida infections. Data on measures of disease severity/outcome and risk factors were abstracted and analyzed to determine differences associated with various Candida species.

Results

Exactly 106 cases of infection were analyzed. Non-albicans species were associated with a significantly longer length of stay postdiagnosis (P=0.03), as well as longer treatment (P=0.02). Candida albicans was associated with a higher number of antihypotensive medications required (P=0.03) and length of mechanical ventilation postdiagnosis (P=0.05). Candida tropicalis was associated with the highest mortality (45.5%). Hypotension, which was found to be significantly associated with concurrent infection, was significantly associated with increased risk of mortality (odds ratio =5.85, P=0.005). Initial choice of antifungal therapy was not associated with differences in eventual patient mortality. Multivariate logistic regression modeling revealed a trend toward C. albicans infection in patients receiving antineoplastic chemotherapy and non-albicans infection in patients with >96 hours mechanical ventilation.

Conclusion

Interspecies differences may exist for Candida in terms of disease severity and risk factors. Underlying morbidity and the role of concurrent infections may play a key role in poor outcomes.

Acknowledgments

The authors would like to acknowledge the invaluable assistance of Drs Bhumi Patel and Tanzina Nashid in abstracting hospital chart data for this study.

This work was supported by funding from the Merck Investigator Initiated Studies Program (grant no 36660). The abstract of this paper was presented at the Society for Healthcare Epidemiology of America Spring 2015 Conference, May 14–17, 2015, Orlando, FL, USA, as a poster presentation (conference abstract no 6526).

Disclosure

The authors report no conflicts of interest in this work.