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人血清可诱导 及草绿色链球菌对达托霉素产生耐受性。

Human serum induces daptomycin tolerance in and viridans group streptococci.

作者信息

Tickle Alicia R H, Ledger Elizabeth V K, Edwards Andrew M

机构信息

MRC Centre for Molecular Bacteriology and Infection, Imperial College London, Armstrong Rd, London, SW7 2AZ, UK.

Southmead Hospital, Southmead Road, Westbury-on-Trym, Bristol, Avon, BS10 5NB, UK.

出版信息

Microbiology (Reading). 2022 Dec;168(12). doi: 10.1099/mic.0.001282.

Abstract

Daptomycin is a membrane-targeting lipopeptide antibiotic used in the treatment of infective endocarditis caused by multidrug-resistant Gram-positive bacteria such as , enterococci and viridans group streptococci. Despite demonstrating excellent activity and a low prevalence of resistant isolates, treatment failure is a significant concern, particularly for enterococcal infection. We have shown recently that human serum triggers daptomycin tolerance in , but it was not clear if a similar phenotype occurred in other major infective endocarditis pathogens. We found that , or grown under standard laboratory conditions were efficiently killed by daptomycin, whereas bacteria pre-incubated in human serum survived exposure to the antibiotic, with >99 % cells remaining viable. Incubation of enterococci or streptococci in serum led to peptidoglycan accumulation, as shown by increased incorporation of the fluorescent d-amino acid analogue HADA. Inhibition of peptidoglycan accumulation using the antibiotic fosfomycin resulted in a >tenfold reduction in serum-induced daptomycin tolerance, demonstrating the important contribution of the cell wall to the phenotype. We also identified a small contribution to daptomycin tolerance in from cardiolipin synthases, although this may reflect the inherent increased susceptibility of cardiolipin-deficient mutants. In summary, serum-induced daptomycin tolerance is a consistent phenomenon between Gram-positive infective endocarditis pathogens, but it may be mitigated using currently available antibiotic combination therapy.

摘要

达托霉素是一种作用于细胞膜的脂肽类抗生素,用于治疗由耐多药革兰氏阳性菌引起的感染性心内膜炎,如粪肠球菌和草绿色链球菌。尽管达托霉素显示出优异的抗菌活性且耐药菌株的发生率较低,但治疗失败仍是一个重大问题,尤其是对于肠球菌感染。我们最近发现,人血清会引发粪肠球菌对达托霉素的耐受性,但尚不清楚在其他主要的感染性心内膜炎病原体中是否会出现类似的表型。我们发现,在标准实验室条件下培养的粪肠球菌、屎肠球菌或草绿色链球菌会被达托霉素有效杀灭,而预先在人血清中孵育的细菌在接触抗生素后仍能存活,超过99%的细胞仍保持活力。如荧光d -氨基酸类似物HADA掺入增加所示,肠球菌或链球菌在血清中孵育会导致肽聚糖积累。使用抗生素磷霉素抑制肽聚糖积累可使血清诱导的达托霉素耐受性降低超过10倍,这表明细胞壁对该表型具有重要作用。我们还发现心磷脂合酶对粪肠球菌的达托霉素耐受性有微小贡献,尽管这可能反映了心磷脂缺陷突变体固有的易感性增加。总之,血清诱导的达托霉素耐受性在革兰氏阳性感染性心内膜炎病原体中是一种一致现象,但使用目前可用的联合抗生素疗法可能会减轻这种现象。

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