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Target for bacteriostatic and bactericidal activities of beta-lactam antibiotics against Escherichia coli resides in different penicillin-binding proteins.

机译:β-内酰胺类抗生素对大肠杆菌的抑菌和杀菌活性的目标位于不同的青霉素结合蛋白中。

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摘要

The relationship between cell-killing kinetics and penicillin-binding protein (PBP) saturation has been evaluated in the permeability mutant Escherichia coli DC2 in which the antimicrobial activity of beta-lactams has been described as being directly related to the extent of saturation of the PBP target(s). Saturation of a single PBP by cefsulodin (PBP 1s), mecillinam (PBP 2), and aztreonam (PBP 3) resulted in a slow rate of killing (2.5-, 1.5-, and 0.8-log-unit decreases in the number of CFU per milliliter, respectively, in 6 h). Saturation of two of the three essential PBPs resulted in a marked increase in the rate of killing, which reached the maximum value when PBPs 1s and 2 were simultaneously saturated by a combination of cefsulodin and mecillinam (4.7-log-unit decrease in the number of CFU per milliliter in 6 h). Inactivation of all three essential PBPs by the combination of cefsulodin, mecillinam, and aztreonam further increased the killing kinetics (5.5-log-unit decrease in the number of CFU per milliliter), and this was not significantly changed upon additional saturation of the nonessential PBPs 5 and 6 by cefoxitin. Similar relationships between PBP saturation and killing kinetics were obtained with imipenem and meropenem at concentrations which inhibited only one PBP (PBP 2), only two PBPs (PBP 1s and 2), or all three essential PBPs. Saturation of one or more PBPs also resulted in a different rate of bacteriolysis, the highest rate being obtained by the cefsulodin-mecillinam combination and by 5 micrograms of either imipenem or meropenem per ml. All of these conditions caused saturation of PBP 2 and saturation or extensive binding of PBP 1s. However, none of these conditions caused determined the fastest possible rate of killing, which occurred only when all three essential PBPs were saturated. It was concluded that the actual killing effect of beta-lactams is reflected by killing rates that approach the fastest possible rate for the given microorganism and that the targets for the bactericidal activity are precisely those PBPs whose saturation or binding occurs under conditions.
机译:已经在通透性突变大肠杆菌DC2中评估了细胞杀灭动力学和青霉素结合蛋白(PBP)饱和度之间的关系,其中β-内酰胺的抗菌活性被描述为与PBP饱和度直接相关。目标。头孢磺啶(PBP 1s),美西林(PBP 2)和氨曲南(PBP 3)使单个PBP饱和会导致缓慢的杀灭速度(CFU数量下降2.5、1.5和0.8 log单位)每毫升,分别在6小时内)。三个必需PBP中的两个饱和会导致杀死率显着增加,当头孢磺啶和美西林同时使PBP 1s和2同时饱和时,杀灭率达到最大值(减少4.7个log单位)。每毫升CFU在6小时内)。头孢磺啶,美西林和aztreonam联合灭活所有三个必需的PBP进一步增加了杀灭动力学(每毫升CFU数量减少了5.5个对数单位),并且当非必需PBP进一步饱和时,这一变化并没有明显改变头孢西丁5和6。亚胺培南和美罗培南在仅抑制一个PBP(PBP 2),仅两个PBP(PBP 1s和2)或全部三个必需PBP的浓度下,获得了PBP饱和度与杀灭动力学之间的相似关系。一种或多种PBP的饱和也会导致不同的细菌分解速率,最高的速率是通过头孢磺啶-美西林组合和每毫升5微克亚胺培南或美罗培南获得的。所有这些条件都导致PBP 2饱和和PBP 1s饱和或广泛结合。但是,这些条件均未导致确定最快的杀灭率,仅在所有三个必需PBP饱和时才会发生。结论是,β-内酰胺类化合物的实际杀灭作用反映在对给定微生物接近最快杀灭率的杀灭率上,而杀菌活性的目标正是那些在一定条件下发生饱和或结合的PBP。

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