首页> 外文OA文献 >Bacteriostatic and bactericidal activities of beta-lactams against Streptococcus (Enterococcus) faecium are associated with saturation of different penicillin-binding proteins.
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Bacteriostatic and bactericidal activities of beta-lactams against Streptococcus (Enterococcus) faecium are associated with saturation of different penicillin-binding proteins.

机译:β-内酰胺类对粪链球菌(肠球菌)的抑菌和杀菌活性与不同青霉素结合蛋白的饱和度有关。

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摘要

The MICs and MBCs of benzylpenicillin, ampicillin, cefotaxime, and methicillin were evaluated against a Streptococcus (Enterococcus) faecium wild-type strain and against three mutants hyperproducing PBP 5 in cells incubated at both optimal and suboptimal temperatures. In the wild-type strain grown at optimal temperature, the MBCs of all beta-lactams were significantly greater than the MICs (bacteriostatic effect). As opposed to this, in the same cells grown at suboptimal temperature and in the mutants hyperproducing PBP 5 at all temperatures, the MICs of all antibiotics coincided with the MBCs (bactericidal effect). Under all conditions in which the MIC and MBC were the same, with all antibiotics, growth inhibition occurred only at the minimal concentration saturating all penicillin-binding proteins (PBPs) (or at higher concentrations). On the contrary, under conditions in which the MIC was lower than the MBC, only some of the PBPs were saturated (or bound) at both the MIC and the MBC, PBP 5 in no case being either saturated or bound. Under all conditions in which saturation of all PBPs was needed for growth inhibition, cells died at all antibiotic MBCs with kinetics which were much faster than those with which they died at the MBCs under conditions in which not all PBPs were saturated (or bound). In addition, under the former conditions, antibiotic concentrations above the MBCs did not significantly accelerate cell death kinetics, while under the latter conditions there was an acceleration in kinetics with increasing antibiotic concentrations up to full saturation of PBPs. It is suggested that the killing that occurs when all PBPs are saturated is a direct consequence of inactivation of PBP functions, while killing occurring when only some of them are saturated or bound is also (or mainly) an indirect consequence of inability of cells to grow and that, in S. faecium, the targets for growth inhibition and cell killing reside in different PBPs: for the latter effect, inactivation of one (or more) of the high-molecular-weight PBPs is sufficient, whereas in the former case inactivation of PBP 5 is necessary (after saturation of all other PBPs).
机译:评估了青霉素,氨苄青霉素,头孢噻肟和甲氧西林的MIC和MBC对粪链球菌(Enterococcus)粪便野生型菌株以及在最佳和次最佳温度下培养的细胞中高产PBP 5的三个突变体的评估。在最佳温度下生长的野生型菌株中,所有β-内酰胺的MBC均明显大于MIC(抑菌作用)。与此相反,在亚最佳温度下生长的相同细胞中以及在所有温度下都高产PBP 5的突变体中,所有抗生素的MIC与MBC一致(杀菌作用)。在所有MIC和MBC均相同的所有条件下,对于所有抗生素,仅在使所有青霉素结合蛋白(PBPs)饱和的最低浓度(或更高浓度)下才会发生生长抑制。相反,在MIC低于MBC的条件下,只有一些PBP在MIC和MBC处都饱和(或结合),而PBP 5在任何情况下都不是饱和或结合。在需要全部PBP饱和以抑制生长的所有条件下,细胞在所有抗生素MBC处的死亡动力学要比在并非所有PBP都饱和(或结合)的条件下在MBC处死亡的动力学快得多。此外,在前一种条件下,MBCs上方的抗生素浓度不会显着加速细胞死亡动力学,而在后一种条件下,随着抗生素浓度的增加直至PBP完全饱和,动力学会加速。建议所有PBP饱和时发生的杀灭是PBP功能失活的直接结果,而只有部分PBP功能饱和或结合时发生的杀灭也(或主要)是细胞无法生长的间接结果。而且,在粪粪链球菌中,抑制生长和杀死细胞的靶点位于不同的PBP中:对于后者的作用,一个(或多个)高分子量PBP的失活就足够了,而在前一种情况下,失活就足够了需要PBP 5的最大值(在所有其他PBP饱和之后)。

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