UMR 1173 INSERM, Université de Versailles-Saint-Quentin-en-Yvelines, Montigny-le-Bretonneux, France.
Laboratoire de Microbiologie, CHU de Caen, Caen, France.
J Antimicrob Chemother. 2018 Apr 1;73(4):981-986. doi: 10.1093/jac/dkx499.
Daptomycin has become a first-line therapeutic option for vancomycin-resistant Enterococcus faecium infective endocarditis (IE). Although high doses (≥8 mg/kg) are often recommended, optimal doses, particularly for strains with MICs close to the susceptibility breakpoint (4 mg/L), are still debated.
Daptomycin efficacy at doses equivalent to 8 mg/kg daptomycin (DAP8) and 12 mg/kg daptomycin (DAP12) in humans was evaluated in a rabbit model of aortic valve IE induced by 108 cfu of E. faecium reference strain Aus0004 (daptomycin MIC = 2 mg/L) or its in vitro mutant strain Mut4 (daptomycin MIC = 4 mg/L). Treatment began 48 h post-inoculation and lasted 5 days.
With Aus0004, the median log10 cfu/g of vegetations was significantly lower after DAP8 and DAP12 versus controls [6.05 (n = 12) and 2.15 (n = 10) versus 9.14 (n = 11), respectively; P < 0.001], with DAP12 being more effective than DAP8 concerning vegetation bacterial load (P < 0.001) and percentages of sterile vegetations (100% versus 0%, respectively; P < 0.001). Daptomycin-resistant Aus0004 mutants were detected in 8.3% of DAP8-treated vegetations. With Mut4, the median log10 cfu/g of vegetations was significantly lower after DAP8 and DAP12 versus controls [7.7 (n = 11) and 6.95 (n = 10) versus 9.59 (n = 11), respectively; P = 0.001 and P = 0.002], without any between-dose difference, but no vegetation was sterile. Moreover, 7 of 11 (63.6%) and 7 of 9 (77.8%) vegetations contained resistant mutants after DAP8 and DAP12, respectively.
DAP12 was the most successful strategy against IE due to a WT E. faecium strain (daptomycin MIC = 2 mg/L). To treat IE strains with MIC = 4 mg/L, DAP8 or DAP12 monotherapy was poorly effective with the risk of resistant mutant emergence. Reassessment of the daptomycin susceptibility breakpoint for enterococci seems necessary.
达托霉素已成为治疗耐万古霉素粪肠球菌感染性心内膜炎(IE)的一线治疗选择。尽管通常推荐使用高剂量(≥8mg/kg),但对于 MIC 接近药敏折点(4mg/L)的菌株,最佳剂量仍存在争议。
在 108cfu粪肠球菌参考菌株 Aus0004(达托霉素 MIC=2mg/L)或其体外突变株 Mut4(达托霉素 MIC=4mg/L)诱导的兔主动脉瓣 IE 模型中,评估了剂量相当于 8mg/kg 达托霉素(DAP8)和 12mg/kg 达托霉素(DAP12)的达托霉素疗效。治疗于接种后 48 小时开始,持续 5 天。
对于 Aus0004,与对照组相比,DAP8 和 DAP12 后,心内膜炎病灶中的中位 log10cfu/g 明显降低[分别为 6.05(n=12)和 2.15(n=10)与 9.14(n=11);P<0.001],DAP12 对病灶细菌负荷(P<0.001)和无菌病灶百分比(100%与 0%,分别;P<0.001)的疗效均优于 DAP8。在 8.3%的 DAP8 治疗病灶中检测到达托霉素耐药的 Aus0004 突变体。对于 Mut4,与对照组相比,DAP8 和 DAP12 后心内膜炎病灶中的中位 log10cfu/g 明显降低[分别为 7.7(n=11)和 6.95(n=10)与 9.59(n=11);P=0.001 和 P=0.002],但剂量之间无差异,但无病灶无菌。此外,在 DAP8 和 DAP12 后,分别有 7/11(63.6%)和 7/9(77.8%)的心内膜炎病灶中含有耐药突变体。
DAP12 是针对 MIC=2mg/L 的 WT 粪肠球菌菌株治疗 IE 的最成功策略。对于 MIC=4mg/L 的 IE 菌株,DAP8 或 DAP12 单药治疗效果不佳,有耐药突变体出现的风险。似乎有必要重新评估肠球菌的达托霉素药敏折点。
