通过溶剂诱导蛋白质沉淀和定量质谱法研究抗感染药物的靶向作用

IF 4 2区 医学 Q2 CHEMISTRY, MEDICINAL
Lorenzo Bizzarri, Dominik Steinbrunn, Thibaut Quennesson, Antoine Lacour, Gabriella Ines Bianchino, Patricia Bravo, Philippe Chaignon, Jonas Lohse, Pascal Mäser, Myriam Seemann, Serge Van Calenbergh, Anna K H Hirsch, Hannes Hahne
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引用次数: 0

摘要

抗菌药耐药性(AMR)对全球健康构成严重威胁。抗药性的迅速出现与抗菌药物开发的缓慢步伐形成了鲜明对比,这凸显了对创新药物发现方法的迫切需求。本研究通过引入整体溶剂诱导蛋白沉淀(iSPP),在接近生理条件下快速评估病原微生物提取物中先导化合物的靶向参与性,从而解决了早期药物开发中的一个关键瓶颈。针对细菌的 iSPP 方法建立在已有的 SPP 程序基础上,具有优化变性梯度和最小化样品输入量的特点。iSPP 工作流程的有效性最初是通过一项多药物靶点接合研究来证明的。利用定量质谱(LC-MS/MS)技术,我们在四种 AMR 相关病原体(三种革兰氏阴性菌大肠埃希菌、肺炎克雷伯氏菌、铜绿假单胞菌和革兰氏阳性菌金黄色葡萄球菌)的细胞提取物中成功鉴定了七种不同抗生素的已知药物靶标。iSPP 方法最终被用于证明基于靶点的药物发现所产生的化合物的靶点参与性。我们采用了五种小分子化合物,它们靶向 2-C- 甲基赤藓醇-4-磷酸(MEP)途径中的三种酶--这是抗感染药物开发的一个前景看好的重点。这项研究展示了 iSPP 在确定抗感染药物靶点方面的适应性和高效性,推动了抗 AMR 药物的早期发现。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Studying Target-Engagement of Anti-Infectives by Solvent-Induced Protein Precipitation and Quantitative Mass Spectrometry.

Antimicrobial resistance (AMR) poses a serious threat to global health. The rapid emergence of resistance contrasts with the slow pace of antimicrobial development, emphasizing the urgent need for innovative drug discovery approaches. This study addresses a critical bottleneck in early drug development by introducing integral solvent-induced protein precipitation (iSPP) to rapidly assess the target-engagement of lead compounds in extracts of pathogenic microorganisms under close-to-physiological conditions. iSPP measures the change in protein stability against solvent-induced precipitation in the presence of ligands. The iSPP method for bacteria builds upon established SPP procedures and features optimized denaturation gradients and minimized sample input amounts. The effectiveness of the iSPP workflow was initially demonstrated through a multidrug target-engagement study. Using quantitative mass spectrometry (LC-MS/MS), we successfully identified known drug targets of seven different antibiotics in cell extracts of four AMR-related pathogens: the three Gram-negative bacteria Escherichia coli, Klebsiella pneumoniae, Pseudomonas aeruginosa and the Gram-positive bacterium Staphylococcus aureus. The iSPP method was ultimately applied to demonstrate target-engagement of compounds derived from target-based drug discovery. We employed five small molecules targeting three enzymes in the 2-C-methyl-d-erythritol 4-phosphate (MEP) pathway─a promising focus for anti-infective drug development. The study showcases iSPP adaptability and efficiency in identifying anti-infective drug targets, advancing early-stage drug discovery against AMR.

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来源期刊
ACS Infectious Diseases
ACS Infectious Diseases CHEMISTRY, MEDICINALINFECTIOUS DISEASES&nb-INFECTIOUS DISEASES
CiteScore
9.70
自引率
3.80%
发文量
213
期刊介绍: ACS Infectious Diseases will be the first journal to highlight chemistry and its role in this multidisciplinary and collaborative research area. The journal will cover a diverse array of topics including, but not limited to: * Discovery and development of new antimicrobial agents — identified through target- or phenotypic-based approaches as well as compounds that induce synergy with antimicrobials. * Characterization and validation of drug target or pathways — use of single target and genome-wide knockdown and knockouts, biochemical studies, structural biology, new technologies to facilitate characterization and prioritization of potential drug targets. * Mechanism of drug resistance — fundamental research that advances our understanding of resistance; strategies to prevent resistance. * Mechanisms of action — use of genetic, metabolomic, and activity- and affinity-based protein profiling to elucidate the mechanism of action of clinical and experimental antimicrobial agents. * Host-pathogen interactions — tools for studying host-pathogen interactions, cellular biochemistry of hosts and pathogens, and molecular interactions of pathogens with host microbiota. * Small molecule vaccine adjuvants for infectious disease. * Viral and bacterial biochemistry and molecular biology.
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