@article{1085b0c0e51b4befbef3e213fa0b2659,
title = "Influence of vancomycin minimum inhibitory concentration on the outcome of methicillin-susceptible Staphylococcus aureus left-sided infective endocarditis treated with antistaphylococcal β-lactam antibiotics: a prospective cohort study by the International Collaboration on Endocarditis",
abstract = "Objectives Left-sided methicillin-susceptible Staphylococcus aureus (MSSA) endocarditis treated with cloxacillin has a poorer prognosis when the vancomycin minimum inhibitory concentration (MIC) is ≥1.5 mg/L. We aimed to validate this using the International Collaboration on Endocarditis cohort and to analyse whether specific genetic characteristics were associated with a high vancomycin MIC (≥1.5 mg/L) phenotype. Methods All patients with left-sided MSSA infective endocarditis treated with antistaphylococcal β-lactam antibiotics between 2000 and 2006 with available isolates were included. Vancomycin MIC was determined by Etest as either high (≥1.5 mg/L) or low (<1.5 mg/L). Isolates underwent spa typing to infer clonal complexes and multiplex PCR for identifying virulence genes. Univariate analysis was performed to evaluate the association between in-hospital and 1-year mortality, and vancomycin MIC phenotype. Results Sixty-two cases met the inclusion criteria. Vancomycin MIC was low in 28 cases (45%) and high in 34 cases (55%). No significant differences in patient demographic data or characteristics of infection were observed between patients with infective endocarditis due to high and low vancomycin MIC isolates. Isolates with high and low vancomycin MIC had similar distributions of virulence genes and clonal lineages. In-hospital and 1-year mortality did not differ significantly between the two groups (32% (9/28) vs. 27% (9/34), p 0.780; and 43% (12/28) vs. 29% (10/34), p 0.298, for low and high vancomycin MIC respectively). Conclusions In this international cohort of patients with left-sided MSSA endocarditis treated with antistaphylococcal β-lactams, vancomycin MIC phenotype was not associated with patient demographics, clinical outcome or virulence gene repertoire.",
keywords = "Endocarditis, Genotype, Phenotype, Staphylococcus aureus, Vancomycin MIC",
author = "{the International Collaboration on Endocarditis Microbiology Investigators} and E. Athan and O. Harris and Korman, {T. M.} and D. Kotsanas and P. Jones and P. Reinbott and S. Ryan and Fortes, {C. Q.} and P. Garcia and Jones, {S. B.} and B. Barsic and S. Bukovski and C. Selton-Suty and N. Aissa and T. Doco-Lecompte and F. Delahaye and F. Vandenesch and P. Tattevin and B. Hoen and P. Plesiat and H. Giamarellou and E. Giannitsioti and E. Tarpatzi and E. Durante-Mangoni and D. Iossa and S. Orlando and Ursi, {M. P.} and Pafundi, {P. C.} and {D{\textquoteright} Amico}, F. and M. Bernardo and S. Cuccurullo and G. Dialetto and Covino, {F. E.} and S. Manduca and {Della Corte}, A. and {De Feo}, M. and Tripodi, {M. F.} and T. Baban and Kanafani, {Z. A.} and Kanj, {S. S.} and J. Sfeir and M. Yasmine and A. Morris and Murdoch, {D. R.} and Premru, {M. M.} and T. Lejko-Zupanc and M. Almela and J. Ambrosioni and M. Azqueta and G. Peterson",
note = "Funding Information: Supported in part by R01-AI068804 and K24-AI093969 (National Institutes of Health (NIH), USA), and by {\textquoteleft}La Marat{\'o} de TV3{\textquoteright} (20152610) Barcelona, Spain; Instituto de Salud Carlos III and the Ministerio de Economia and Competitividad (FIS PI14/00603), Madrid, Spain; and a 2016 European Society of Clinical Microbiology and Infectious Diseases (ESCMID) research grant. JMP received a {\textquoteleft}Rio Hortega{\textquoteright} research grant (CM14/00135, 2015–16) from Instituto de Salud Carlos III and the Ministerio de Economia and Competitividad, Madrid, Spain, and a ESCMID/FEMS Joint Research Fellowship Award (2016). Instituto de Salud Carlos III, Ministerio de Econom{\'i}a y Competitividad, Madrid, Spain, provided to JMM a personal intensification research grant (INT15/00168 during 2016). VGF reports the following potential conflicts of interest: chair of the Scientific Advisory Board for Merck V710; paid consultant for Pfizer, Novartis, Galderma, Novadigm, Durata, Debiopharm, Genentech, Achaogen, Affinium, Medicines Co., Cerexa, Tetraphase, Trius, MedImmune, Bayer, Theravance, Cubist, Basilea and Affinergy; grants pending from MedImmune, Actavis/Forest/Cerexa, Pfizer, Merck/Cubist, Advanced Liquid Logics, Theravance, Novartis, Medical Surfaces, and Locus Biotechnology; royalties from UpToDate; personal fees for development or presentation of educational presentations (Green Cross, Cubist, Cerexa, Durata, Theravance), outside the submitted work; and patent pending related to sepsis diagnostics. JMM has received consulting honoraria and/or research grants from AbbVie, Bristol-Myers Squibb, Cubist, Novartis, Gilead Sciences and ViiV. The other authors report no conflicts of interest relevant to this article. Publisher Copyright: {\textcopyright} 2017 European Society of Clinical Microbiology and Infectious Diseases",
year = "2017",
month = aug,
doi = "10.1016/j.cmi.2017.01.017",
language = "English (US)",
volume = "23",
pages = "544--549",
journal = "Clinical Microbiology and Infection",
issn = "1198-743X",
publisher = "Elsevier Limited",
number = "8",
}