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筛选 NCI 多样性集 V 以获得抗耐甲氧西林金黄色葡萄球菌活性:头孢西丁协同作用和 LC-MS/MS 确认叶酸/胸苷生物合成抑制。

Screening the NCI diversity set V for anti-MRSA activity: cefoxitin synergy and LC-MS/MS confirmation of folate/thymidine biosynthesis inhibition.

机构信息

Division of Pharmacology and Pharmaceutical Sciences, School of Pharmacy, University of Missouri-Kansas City , Kansas City, Missouri, USA.

出版信息

Microbiol Spectr. 2023 Dec 12;11(6):e0054123. doi: 10.1128/spectrum.00541-23. Epub 2023 Oct 27.

Abstract

New antibacterial agents are urgently needed to counter increasingly resistant bacteria. One approach to this problem is library screening for new antibacterial agents. Library screening efforts can be improved by increasing the information content of the screening effort. In this study, we screened the National Cancer Institute diversity set V against methicillin-resistant (MRSA) with several enhancements. One of these is to screen the library before and after microsomal metabolism as means to identify potential active metabolites. A second enhancement is to screen the library in the absence and presence of sub-minimum inhibitory concentration levels of another antibiotic, such as cefoxitin in this study. This identified four agents with synergistic activity with cefoxitin out of 16 agents with good MRSA activity alone. Finally, active agents from this effort were counter-screened in the presence of thymidine, which quickly identified three folate/thymidine biosynthesis inhibitors, and also screened for bactericidal vs bacteriostatic activity.

摘要

急需新型抗菌药物来对抗日益耐药的细菌。解决这个问题的一种方法是针对新型抗菌药物进行文库筛选。通过增加筛选工作的信息量,可以提高文库筛选的效果。在这项研究中,我们对国家癌症研究所多样性集合 V 进行了筛选,以检测耐甲氧西林金黄色葡萄球菌(MRSA),并进行了几项增强。其中之一是在进行和不进行微粒体代谢之前和之后筛选文库,作为识别潜在的活性代谢物的方法。另一个增强是在亚最低抑制浓度水平的另一种抗生素(如本研究中的头孢西丁)存在和不存在的情况下筛选文库。从单独对 MRSA 有良好活性的 16 种药物中,筛选出了 4 种与头孢西丁具有协同作用的药物。最后,在胸腺嘧啶存在的情况下对来自这一研究的活性药物进行了反向筛选,这很快确定了三种叶酸/胸腺嘧啶生物合成抑制剂,并对杀菌和抑菌活性进行了筛选。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2b95/10715016/65b6bb5b1471/spectrum.00541-23.f001.jpg

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