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基于片段的细菌DnaG-SSB相互作用抑制剂的发现

Fragment-Based Discovery of Inhibitors of the Bacterial DnaG-SSB Interaction.

作者信息

Chilingaryan Zorik, Headey Stephen J, Lo Allen T Y, Xu Zhi-Qiang, Otting Gottfried, Dixon Nicholas E, Scanlon Martin J, Oakley Aaron J

机构信息

Molecular Horizons and School of Chemistry, University of Wollongong, and Illawarra Health and Medical Research Institute, Wollongong, NSW 2522, Australia.

Monash Institute of Pharmaceutical Sciences, Monash University, Parkville, VIC 3052, Australia.

出版信息

Antibiotics (Basel). 2018 Feb 22;7(1):14. doi: 10.3390/antibiotics7010014.

Abstract

In bacteria, the DnaG primase is responsible for synthesis of short RNA primers used to initiate chain extension by replicative DNA polymerase(s) during chromosomal replication. Among the proteins with which DnaG interacts is the single-stranded DNA-binding protein, SSB. The C-terminal hexapeptide motif of SSB (DDDIPF; SSB-Ct) is highly conserved and is known to engage in essential interactions with many proteins in nucleic acid metabolism, including primase. Here, fragment-based screening by saturation-transfer difference nuclear magnetic resonance (STD-NMR) and surface plasmon resonance assays identified inhibitors of the primase/SSB-Ct interaction. Hits were shown to bind to the SSB-Ct-binding site using N-¹H HSQC spectra. STD-NMR was used to demonstrate binding of one hit to other SSB-Ct binding partners, confirming the possibility of simultaneous inhibition of multiple protein/SSB interactions. The fragment molecules represent promising scaffolds on which to build to discover new antibacterial compounds.

摘要

在细菌中,DnaG引发酶负责合成短RNA引物,这些引物用于在染色体复制过程中由复制性DNA聚合酶启动链延伸。与DnaG相互作用的蛋白质之一是单链DNA结合蛋白SSB。SSB的C末端六肽基序(DDDIPF;SSB-Ct)高度保守,已知它与核酸代谢中的许多蛋白质(包括引发酶)进行重要的相互作用。在这里,通过饱和转移差异核磁共振(STD-NMR)和表面等离子体共振分析进行的基于片段的筛选确定了引发酶/SSB-Ct相互作用的抑制剂。使用N-¹H HSQC光谱显示命中物与SSB-Ct结合位点结合。STD-NMR用于证明一种命中物与其他SSB-Ct结合伙伴的结合,证实了同时抑制多种蛋白质/SSB相互作用的可能性。这些片段分子代表了有前景的支架,可在此基础上发现新的抗菌化合物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2169/5872125/b3c08d401ead/antibiotics-07-00014-g001.jpg

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