Impact of High-Level Daptomycin Resistance in the Streptococcus mitis Group on Virulence and Survivability during Daptomycin Treatment in Experimental Infective Endocarditis

Author:

Garcia-de-la-Maria C.1,Xiong Y. Q.23,Pericas J. M.1,Armero Y.1,Moreno A.1,Mishra N. N.23,Rybak M. J.4,Tran T. T.5,Arias C. A.5,Sullam P. M.6,Bayer A. S.23,Miro J. M.1

Affiliation:

1. Hospital Clinic-IDIBAPS, University of Barcelona, Barcelona, Spain

2. LA Biomedical Research Institute, Torrance, California, USA

3. Geffen School of Medicine at UCLA, Los Angeles, California, USA

4. Anti-Infective Research Laboratory, Wayne State University, Detroit, Michigan, USA

5. University of Texas School of Medicine, Houston, Texas, USA

6. Veterans Affairs Medical Center and the University of California, San Francisco, California, USA

Abstract

ABSTRACT Among the viridans group streptococci, the Streptococcus mitis group is the most common cause of infective endocarditis. These bacteria have a propensity to be β-lactam resistant, as well as to rapidly develop high-level and durable resistance to daptomycin (DAP). We compared a parental, daptomycin-susceptible (DAP s ) S. mitis/S. oralis strain and its daptomycin-resistant (DAP r ) variant in a model of experimental endocarditis in terms of (i) their relative fitness in multiple target organs in this model (vegetations, kidneys, spleen) when animals were challenged individually and in a coinfection strategy and (ii) their survivability during therapy with daptomycin-gentamicin (an in vitro combination synergistic against the parental strain). The DAP r variant was initially isolated from the cardiac vegetations of animals with experimental endocarditis caused by the parental DAP s strain following treatment with daptomycin. The parental strain and the DAP r variant were comparably virulent when animals were individually challenged. In contrast, in the coinfection model without daptomycin therapy, at both the 10 6 - and 10 7 -CFU/ml challenge inocula, the parental strain outcompeted the DAP r variant in all target organs, especially the kidneys and spleen. When the animals in the coinfection model of endocarditis were treated with DAP-gentamicin, the DAP s strain was completely eliminated, while the DAP r variant persisted in all target tissues. These data underscore that the acquisition of DAP r in S. mitis/S. oralis does come at an intrinsic fitness cost, although this resistance phenotype is completely protective against therapy with a potentially synergistic DAP regimen.

Funder

Department of Veterans Affairs and National Institutes of Health

HHS | National Institutes of Health

MINECO | Instituto de Salud Carlos III

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology

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