基于激酶抑制剂支架的文库高通量筛选抗结核分枝杆菌 H37Rv。
High throughput screening of a library based on kinase inhibitor scaffolds against Mycobacterium tuberculosis H37Rv.
机构信息
Southern Research Institute, 2000 Ninth Avenue South, Birmingham, AL 35205, USA.
出版信息
Tuberculosis (Edinb). 2012 Jan;92(1):72-83. doi: 10.1016/j.tube.2011.05.005. Epub 2011 Jun 25.
Abstract
Kinase targets are being pursued in a variety of diseases beyond cancer, including immune and metabolic as well as viral, parasitic, fungal and bacterial. In particular, there is a relatively recent interest in kinase and ATP-binding targets in Mycobacterium tuberculosis in order to identify inhibitors and potential drugs for essential proteins that are not targeted by current drug regimens. Herein, we report the high throughput screening results for a targeted library of approximately 26,000 compounds that was designed based on current kinase inhibitor scaffolds and known kinase binding sites. The phenotypic data presented herein may form the basis for selecting scaffolds/compounds for further enzymatic screens against specific kinase or other ATP-binding targets in Mycobacterium tuberculosis based on the apparent activity against the whole bacteria in vitro.
摘要
激酶靶标不仅在癌症领域,还在免疫、代谢以及病毒、寄生虫、真菌和细菌等其他疾病领域得到了广泛研究。特别是,人们最近对结核分枝杆菌中的激酶和 ATP 结合靶标产生了浓厚兴趣,以期发现针对当前药物方案未涉及的必需蛋白的抑制剂和潜在药物。在此,我们报告了一个基于当前激酶抑制剂骨架和已知激酶结合位点设计的约 26000 种化合物的靶向文库的高通量筛选结果。本文呈现的表型数据可能为选择进一步针对结核分枝杆菌中特定激酶或其他 ATP 结合靶标的酶筛选的骨架/化合物提供依据,这些筛选是基于化合物对体外全菌的明显活性。
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