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抗菌肽的接种效应。

Inoculum effect of antimicrobial peptides.

机构信息

Laboratory affiliated to Pasteur Italia-Fondazione Cenci Bolognetti, Department of Biochemical Sciences, Sapienza University of Rome, 00185 Rome, Italy.

Department of Chemical Science and Technologies, University of Rome Tor Vergata, 00133 Rome, Italy.

出版信息

Proc Natl Acad Sci U S A. 2021 May 25;118(21). doi: 10.1073/pnas.2014364118.

Abstract

The activity of many antibiotics depends on the initial density of cells used in bacterial growth inhibition assays. This phenomenon, termed the inoculum effect, can have important consequences for the therapeutic efficacy of the drugs, because bacterial loads vary by several orders of magnitude in clinically relevant infections. Antimicrobial peptides are a promising class of molecules in the fight against drug-resistant bacteria because they act mainly by perturbing the cell membranes rather than by inhibiting intracellular targets. Here, we report a systematic characterization of the inoculum effect for this class of antibacterial compounds. Minimum inhibitory concentration values were measured for 13 peptides (including all-D enantiomers) and peptidomimetics, covering more than seven orders of magnitude in inoculated cell density. In most cases, the inoculum effect was significant for cell densities above the standard inoculum of 5 × 10 cells/mL, while for lower densities the active concentrations remained essentially constant, with values in the micromolar range. In the case of membrane-active peptides, these data can be rationalized by considering a simple model, taking into account peptide-cell association, and hypothesizing that a threshold number of cell-bound peptide molecules is required in order to cause bacterial killing. The observed effect questions the clinical utility of activity and selectivity determinations performed at a fixed, standardized cell density. A routine evaluation of the dependence of the activity of antimicrobial peptides and peptidomimetics on the inoculum should be considered.

摘要

许多抗生素的活性取决于用于细菌生长抑制测定的初始细胞密度。这种现象被称为接种效应,它可能对抗菌药物的治疗效果产生重要影响,因为在临床相关感染中,细菌负荷的数量级可以相差几个数量级。抗菌肽是对抗耐药菌的一类有前途的分子,因为它们主要通过扰乱细胞膜而不是抑制细胞内靶标来发挥作用。在这里,我们系统地描述了这类抗菌化合物的接种效应。我们测量了 13 种肽(包括全 D 对映体)和肽类似物的最小抑菌浓度值,涵盖了接种细胞密度超过七个数量级的范围。在大多数情况下,接种效应在细胞密度高于标准接种密度 5×10 个细胞/ml 时非常显著,而在较低的密度下,活性浓度基本保持不变,在微摩尔范围内。对于膜活性肽,通过考虑一个简单的模型,考虑肽-细胞的结合,并假设需要一个细胞结合的肽分子的阈值数量才能引起细菌杀伤,可以合理地解释这些数据。观察到的效应质疑了在固定、标准化细胞密度下进行的活性和选择性测定的临床实用性。应该考虑常规评估抗菌肽和肽类似物的活性对接种的依赖性。

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