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抗生素穿过革兰氏阴性菌外膜的摄取:更精准的预测助力研发更优抗生素。

Antibiotic Uptake Across Gram-Negative Outer Membranes: Better Predictions Towards Better Antibiotics.

作者信息

Ferreira Ricardo J, Kasson Peter M

机构信息

Science for Life Laboratory, Department of Cell and Molecular Biology , Uppsala University , Box 596, 75124 Uppsala , Sweden.

Departments of Biomedical Engineering and Molecular Physiology and Biological Physics , University of Virginia , Box 800886, Charlottesville , Virginia 22908 , United States.

出版信息

ACS Infect Dis. 2019 Dec 13;5(12):2096-2104. doi: 10.1021/acsinfecdis.9b00201. Epub 2019 Oct 25.

DOI:10.1021/acsinfecdis.9b00201
PMID:31593635
Abstract

Crossing the Gram-negative bacterial membrane poses a major barrier to antibiotic development, as many small molecules that can biochemically inhibit key bacterial processes are rendered microbiologically ineffective by their poor cellular uptake. The outer membrane is the major permeability barrier for many drug-like molecules, and the chemical properties that enable efficient uptake into mammalian cells fail to predict bacterial uptake. We have developed a computational method for accurate prospective prediction of outer membrane uptake of drug-like molecules, which we combine with a new medium-throughput experimental assay of outer membrane vesicle swelling. Parallel molecular dynamics simulations of compound uptake through () OmpF are used to successfully and quantitatively predict experimental permeabilities measured via either outer membrane swelling or prior liposome-swelling measurements. These simulations are analyzed using an inhomogeneous solubility-diffusion model to yield predictions of permeability. For most polar molecules we test, outer membrane permeability also correlates well with whole-cell uptake. The ability to accurately predict and measure outer membrane uptake of a wide variety of small molecules will enable simpler determination of which molecular scaffolds and which derivatives are most promising prior to extensive chemical synthesis. It will also assist in formulating a more systematic understanding of the chemical determinants of outer membrane permeability.

摘要

跨越革兰氏阴性菌细胞膜是抗生素研发的一个主要障碍,因为许多能够在生化层面抑制关键细菌过程的小分子,由于其较差的细胞摄取能力而在微生物学上无效。外膜是许多类药物分子的主要渗透屏障,那些能够使药物有效进入哺乳动物细胞的化学性质并不能预测其进入细菌细胞的能力。我们已经开发出一种计算方法,用于准确前瞻性预测类药物分子的外膜摄取情况,并将其与一种新的外膜囊泡肿胀的中通量实验测定方法相结合。通过()OmpF进行化合物摄取的平行分子动力学模拟被用于成功且定量地预测通过外膜肿胀或先前的脂质体肿胀测量所测得的实验渗透率。这些模拟通过非均匀溶解度-扩散模型进行分析,以得出渗透率的预测结果。对于我们测试的大多数极性分子,外膜渗透率与全细胞摄取也有很好的相关性。准确预测和测量各种小分子外膜摄取的能力,将能够在进行广泛化学合成之前,更简单地确定哪些分子支架和哪些衍生物最有前景。这也将有助于更系统地理解外膜渗透率的化学决定因素。

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