Changing Characteristics of Staphylococcus aureus Bacteremia: Results From a 21-Year, Prospective, Longitudinal Study | Zendy

Maria Souli | Zendy; Felicia Ruffin | Zendy; Seong-Ho Choi | Zendy; Lawrence P. Park | Zendy; Shengli Gao | Zendy; Nicholas Lent | Zendy; Batu K. SharmaKuinkel | Zendy; Joshua T. Thaden | Zendy; Stacey A. Maskarinec | Zendy; Lisa Wanda | Zendy; Jonathan Hill-Rorie | Zendy; Bobby Warren | Zendy; Brenda Hansen | Zendy; Vance G. Fowler | Zendy

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Changing Characteristics of Staphylococcus aureus Bacteremia: Results From a 21-Year, Prospective, Longitudinal Study

Author(s) -

Maria Souli,

Felicia Ruffin,

Seong-Ho Choi,

Lawrence P. Park,

Shengli Gao,

Nicholas Lent,

Batu K. SharmaKuinkel,

Joshua T. Thaden,

Stacey A. Maskarinec,

Lisa Wanda,

Jonathan Hill-Rorie,

Bobby Warren,

Brenda Hansen,

Vance G. Fowler

Publication year - 2019

Publication title -

clinical infectious diseases

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 3.44

H-Index - 336

eISSN - 1537-6591

pISSN - 1058-4838

DOI - 10.1093/cid/ciz112

Subject(s) - medicine , bacteremia , staphylococcus aureus , prospective cohort study , staphylococcal infections , micrococcaceae , microbiology and biotechnology , antibiotics , bacteria , genetics , biology

Background We conducted a longitudinal study to evaluate changes in the clinical presentation and epidemiology of Staphylococcus aureus bacteremia (SAB) in an academic, US medical center. Methods Consecutive patients with monomicrobial SAB were enrolled from January 1995 to December 2015. Each person’s initial bloodstream S. aureus isolate was genotyped using spa typing. Clonal complexes (CCs) were assigned using Ridom StaphType software. Changes over time in both the patient and bacterial characteristics were estimated with linear regression. Associations between genotypes or clinical characteristics and complications were estimated using multivariable regression models. Results Among the 2348 eligible participants, 54.2% had an implantable, foreign body of some type. This proportion increased significantly during the 21-year study period, by 0.96% annually (P = .002), as did comorbid conditions and acquisition outside of the hospital. Rates of any metastatic complication also significantly increased, by 0.94% annually (P = .019). Among the corresponding bloodstream S. aureus isolates, spa-CC012 (multi-locus sequence type [MLST] CC30), -CC004 (MLST CC45), -CC189 (MLST CC1), and -CC084 (MLST CC15) all significantly declined during the study period, while spa-CC008 (MLST CC8) significantly increased. Patients with SAB due to spa-CC008 were significantly more likely to develop metastatic complications in general, and abscesses, septic emboli, and persistent bacteremia in particular. After adjusting for demographic, racial, and clinical variables, the USA300 variant of spa-CC008 was independently associated with metastatic complications (odds ratio 1.42; 95% confidence interval 1.02–1.99). Conclusions Systematic approaches for monitoring complications of SAB and genotyping the corresponding bloodstream isolates will help identify the emergence of hypervirulent clones and likely improve clinical management of this syndrome.

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