CHEMOPROPHYLACTIC EFFICACY AGAINST EXPERIMENTAL ENDOCARDITIS CAUSED BY BETA-LACTAMASE-PRODUCING, AMINOGLYCOSIDE-RESISTANT ENTEROCOCCI IS ASSOCIATED WITH PROLONGED SERUM INHIBITORY ACTIVITY

We studied the prevention of experimental aortic endocarditis caused by a β-lactamase-producing, aminoglycoside-resistant strain of Enterococcus faecalis (HH22) in 146 catheterized rabbits. Both vancomycin and ampicillin-sulbactam readily killed this resistant enterococcus strain in vitro. At a challenge inoculum of ~109 CFU, vancomycin (40 mg/kg intravenously [i.v.]), ampicillin (40 mg/kg i.v.), or a combination of ampicillin plus a β-lactamase inhibitor, sulbactam (20 mg/kg, i.v.), did not prevent the development of endocarditis in any of the animals, although mean intravegetation bacterial densities were significantly lower in animals that received vancomycin than they were in animals that received other theapies (P < 0.001). At a challenge inoculum of 106 CFU, vancomycin was 100% effective in preventing enterococcal endocarditis compared with ampicillin (29%; P < 0.00001) and ampicillin-sulbactam (65%; P < 0.01). Factors associated with the superior prophylactic efficacy of vancomycin in this model included prolonged serum inhibitory activity and time above MICs. Factors not associated with the antienterococcal prophylactic efficacy of vancomycin included the duration of the in vitro postantibiotic effect of the drug and the magnitude of the ability of this drug to enhance enterococcal in vitro opsonophagocytic killing by polymorphonuclear leukocytes. The superior prophylactic efficacy of vancomycin in this endocarditis model related to the superior pharmacokinetic profile of the drug when it was given intermittently at dose intervals of every 6 h.