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应激反应途径小分子抑制剂的分析方法开发与高通量筛选

Assay development and high-throughput screening for small molecule inhibitors of a stress response pathway.

作者信息

Stanbery Laura, Matson Jyl S

机构信息

Department of Medical Microbiology and Immunology, College of Medicine and Life Sciences, The University of Toledo, Toledo, OH, USA.

出版信息

Drug Des Devel Ther. 2017 Sep 19;11:2777-2785. doi: 10.2147/DDDT.S144391. eCollection 2017.

Abstract

Antibiotics are important adjuncts to oral rehydration therapy in cholera disease management. However, due to the rapid emergence of resistance to the antibiotics used to treat cholera, therapeutic options are becoming limited. Therefore, there is a critical need to develop additional therapeutics to aid in the treatment of cholera. Previous studies showed that the extracytoplasmic stress response (σ) pathway of is required for full virulence of the organism. The pathway is also required for bacterial growth in the presence of ethanol. Therefore, we exploited this ethanol sensitivity phenotype in order to develop a screen for inhibitors of the pathway, with the aim of also inhibiting virulence of the pathogen. Here we describe the optimization and implementation of our high-throughput screening strategy. From a primary screen of over 100,000 compounds, we have identified seven compounds that validated the growth phenotypes from the primary and counterscreens. These compounds have the potential to be developed into therapeutic agents for cholera and will also be valuable probes for uncovering basic molecular mechanisms of an important cause of diarrheal disease.

摘要

抗生素是霍乱疾病管理中口服补液疗法的重要辅助手段。然而,由于用于治疗霍乱的抗生素耐药性迅速出现,治疗选择变得有限。因此,迫切需要开发更多的治疗方法来辅助霍乱的治疗。先前的研究表明,该菌的胞外应激反应(σ)途径是其完全毒力所必需的。在有乙醇存在的情况下,该途径对于细菌生长也是必需的。因此,我们利用这种乙醇敏感性表型来开发针对该途径抑制剂的筛选方法,目的是同时抑制病原体的毒力。在此,我们描述了我们高通量筛选策略的优化和实施。从对超过100,000种化合物的初步筛选中,我们鉴定出了七种化合物,这些化合物验证了初步筛选和复筛中的生长表型。这些化合物有潜力被开发成霍乱治疗药物,并且对于揭示腹泻病一个重要病因的基本分子机制也将是有价值的探针。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a4e6/5614740/2e0af64d379e/dddt-11-2777Fig1.jpg

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