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首页> 外文期刊>Antimicrobial agents and chemotherapy. >Activities of fosfomycin and rifampin on planktonic and adherent Enterococcus faecalis strains in an experimental foreign-body infection model
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Activities of fosfomycin and rifampin on planktonic and adherent Enterococcus faecalis strains in an experimental foreign-body infection model

机译:磷霉素和利福平在实验性异物感染模型中对浮游性和粘附性粪肠球菌菌株的活性

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Enterococcal implant-associated infections are difficult to treat because antibiotics generally lack activity against enterococcal biofilms. We investigated fosfomycin, rifampin, and their combinations against planktonic and adherent Enterococcus faecalis (ATCC 19433) in vitro and in a foreign-body infection model. The MIC/MBClog values were 32/512 μg/ml for fosfomycin, 4/64 μg/ml for rifampin, 1/2 μg/ml for ampicillin, 2/256 μg/ml for linezolid, 16/32 μg/ml for gentamicin, 1/64 μg/ml for vancomycin, and 1/5 μg/ml for daptomycin. In time-kill studies, fosfomycin was bactericidal at 8x and 16x MIC, but regrowth of resistant strains occurred after 24 h. With the exception of gentamicin, no complete inhibition of growth-related heat production was observed with other antimicrobials on early (3 h) or mature (24 h) biofilms. In the animal model, fosfomycin alone or in combination with daptomycin reduced planktonic counts by ≈4 log 10 CFU/ml below the levels before treatment. Fosfomycin cleared planktonic bacteria from 74% of cage fluids (i.e., no growth in aspirated fluid) and eradicated biofilm bacteria from 43% of cages (i.e., no growth from removed cages). In combination with gentamicin, fosfomycin cleared 77% and cured 58% of cages; in combination with vancomycin, fosfomycin cleared 33% and cured 18% of cages; in combination with daptomycin, fosfomycin cleared 75% and cured 17% of cages. Rifampin showed no activity on planktonic or adherent E. faecalis, whereas in combination with daptomycin it cured 17% and with fosfomycin it cured 25% of cages. Emergence of fosfomycin resistance was not observed in vivo. In conclusion, fosfomycin showed activity against planktonic and adherent E. faecalis. Its role against enterococcal biofilms should be further investigated, especially in combination with rifampin and/or daptomycin treatment.
机译:肠球菌植入物相关的感染很难治疗,因为抗生素通常缺乏针对肠球菌生物膜的活性。我们在体外和异物感染模型中研究了磷霉素,利福平及其组合对浮游性和粘附性粪肠球菌(ATCC 19433)的影响。磷霉素的MIC / MBClog值为32 /> 512μg/ ml,利福平为4 /> 64μg/ ml,氨苄西林为1/2μg/​​ ml,利奈唑胺为2 /> 256μg/ ml,16/32μg/庆大霉素为1毫升,万古霉素为1 /> 64微克/毫升,达托霉素为1/5微克/毫升。在时间杀灭研究中,磷霉素在8倍和16倍MIC时具有杀菌作用,但耐药菌株的再生在24小时后发生。除庆大霉素外,在早期(3 h)或成熟(24 h)生物膜上未观察到其他抗菌剂对生长相关热量产生的完全抑制。在动物模型中,单独使用磷霉素或与达托霉素合用时,可使浮游生物计数降低约4 log 10 CFU / ml,低于治疗前的水平。磷霉素从74%的笼子液中清除了浮游细菌(即吸出液中无生长),从43%的笼子中清除了生物膜细菌(即从移开的笼子中无菌生长)。与庆大霉素合用时,磷霉素清除了77%的笼子,治愈了58%的笼子;与万古霉素合用时,磷霉素清除了33%的笼子,治愈了18%的笼子;与达托霉素合用时,磷霉素清除了75%的笼子,治愈了17%的笼子。利福平对浮游或黏附的粪肠球菌无活性,而与达托霉素合用可治愈17%,与磷霉素合用可治愈25%的笼子。在体内未观察到磷霉素抗性的出现。总之,磷霉素显示出对浮游性和粘附性粪肠球菌的活性。应进一步研究其对肠球菌生物膜的作用,特别是与利福平和/或达托霉素联合治疗。

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