Difficult-to-Treat Resistance in Gram-negative Bacteremia at 173 US Hospitals: Retrospective Cohort Analysis of Prevalence, Predictors, and Outcome of Resistance to All First-line Agents

Sameer S. Kadri; Jennifer Adjemian; Yi Ling Lai; Alicen B. Spaulding; Emily Ricotta; D. Rebecca Prevots; Tara N. Palmore; Chanu Rhee; Michael Klompas; John P. Dekker; John H. Powers; Anthony F. Suffredini; David C. Hooper; Scott K. Fridkin; Robert L. Danner

doi:10.1093/cid/ciy378

Difficult-to-Treat Resistance in Gram-negative Bacteremia at 173 US Hospitals: Retrospective Cohort Analysis of Prevalence, Predictors, and Outcome of Resistance to All First-line Agents

Sameer S. Kadri(Harvard University), Jennifer Adjemian(National Institutes of Health), Yi Ling Lai(National Institutes of Health), Alicen B. Spaulding(National Institutes of Health), Emily Ricotta(National Institutes of Health), D. Rebecca Prevots(National Institutes of Health), Tara N. Palmore(National Institutes of Health Clinical Center), Chanu Rhee(Brigham and Women's Hospital), Michael Klompas(Brigham and Women's Hospital), John P. Dekker(National Institutes of Health Clinical Center), John H. Powers(Leidos (United States)), Anthony F. Suffredini(National Institutes of Health Clinical Center), David C. Hooper(Harvard University), Scott K. Fridkin(Centers for Disease Control and Prevention), Robert L. Danner(National Institutes of Health Clinical Center)

Clinical Infectious Diseases

May 8, 2018

10.1093/cid/ciy378

Cited by 561Open Access

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Abstract

Background: Resistance to all first-line antibiotics necessitates the use of less effective or more toxic "reserve" agents. Gram-negative bloodstream infections (GNBSIs) harboring such difficult-to-treat resistance (DTR) may have higher mortality than phenotypes that allow for ≥1 active first-line antibiotic. Methods: The Premier Database was analyzed for inpatients with select GNBSIs. DTR was defined as intermediate/resistant in vitro to all ß-lactam categories, including carbapenems and fluoroquinolones. Prevalence and aminoglycoside resistance of DTR episodes were compared with carbapenem-resistant, extended-spectrum cephalosporin-resistant, and fluoroquinolone-resistant episodes using CDC definitions. Predictors of DTR were identified. The adjusted relative risk (aRR) of mortality was examined for DTR, CDC-defined phenotypes susceptible to ≥1 first-line agent, and graded loss of active categories. Results: Between 2009-2013, 471 (1%) of 45011 GNBSI episodes at 92 (53.2%) of 173 hospitals exhibited DTR, ranging from 0.04% for Escherichia coli to 18.4% for Acinetobacter baumannii. Among patients with DTR, 79% received parenteral aminoglycosides, tigecycline, or colistin/polymyxin-B; resistance to all aminoglycosides occurred in 33%. Predictors of DTR included urban healthcare and higher baseline illness. Crude mortality for GNBSIs with DTR was 43%; aRR was higher for DTR than for carbapenem-resistant (1.2; 95% confidence interval, 1.0-1.4; P = .02), extended-spectrum cephalosporin-resistant (1.2; 1.1-1.4; P = .001), or fluoroquinolone-resistant (1.2; 1.0-1.4; P = .008) infections. The mortality aRR increased 20% per graded loss of active first-line categories, from 3-5 to 1-2 to 0. Conclusion: Nonsusceptibility to first-line antibiotics is associated with decreased survival in GNBSIs. DTR is a simple bedside prognostic measure of treatment-limiting coresistance.

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