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单细菌细胞水平下抗生素摄取的显微光谱分析见解

Microspectrometric insights on the uptake of antibiotics at the single bacterial cell level.

作者信息

Cinquin Bertrand, Maigre Laure, Pinet Elizabeth, Chevalier Jacqueline, Stavenger Robert A, Mills Scott, Réfrégiers Matthieu, Pagès Jean-Marie

机构信息

DISCO beamline, Synchrotron Soleil, Saint-Aubin, France.

UMR-MD1, Aix-Marseille Université, IRBA, Marseille, France.

出版信息

Sci Rep. 2015 Dec 11;5:17968. doi: 10.1038/srep17968.

Abstract

Bacterial multidrug resistance is a significant health issue. A key challenge, particularly in Gram-negative antibacterial research, is to better understand membrane permeation of antibiotics in clinically relevant bacterial pathogens. Passing through the membrane barrier to reach the required concentration inside the bacterium is a pivotal step for most antibacterials. Spectrometric methodology has been developed to detect drugs inside bacteria and recent studies have focused on bacterial cell imaging. Ultimately, we seek to use this method to identify pharmacophoric groups which improve penetration, and therefore accumulation, of small-molecule antibiotics inside bacteria. We developed a method to quantify the time scale of antibiotic accumulation in living bacterial cells. Tunable ultraviolet excitation provided by DISCO beamline (synchrotron Soleil) combined with microscopy allows spectroscopic analysis of the antibiotic signal in individual bacterial cells. Robust controls and measurement of the crosstalk between fluorescence channels can provide real time quantification of drug. This technique represents a new method to assay drug translocation inside the cell and therefore incorporate rational drug design to impact antibiotic uptake.

摘要

细菌的多重耐药性是一个重大的健康问题。一个关键挑战,尤其是在革兰氏阴性菌抗菌研究中,是要更好地了解抗生素在临床相关细菌病原体中的膜渗透情况。对于大多数抗菌药物来说,穿过膜屏障以在细菌内部达到所需浓度是一个关键步骤。已经开发了光谱测定方法来检测细菌内部的药物,并且最近的研究集中在细菌细胞成像上。最终,我们试图利用这种方法来识别能够改善小分子抗生素在细菌内部的渗透进而积累的药效基团。我们开发了一种方法来量化抗生素在活细菌细胞中的积累时间尺度。由DISCO光束线(同步加速器太阳)提供的可调谐紫外线激发与显微镜相结合,能够对单个细菌细胞中的抗生素信号进行光谱分析。稳健的对照以及荧光通道之间串扰的测量可以提供药物的实时定量。这项技术代表了一种测定细胞内药物转运的新方法,因此可以将合理的药物设计纳入其中以影响抗生素的摄取。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9503/4675965/6b488b3a5628/srep17968-f1.jpg

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