Fragment-Based De Novo Design Reveals a Small-Molecule Inhibitor of Helicobacter Pylori HtrA

Perna Anna M.; Rodrigues Tiago; Schmidt Thomas P.; Boehm Manja; Stutz Katharina; Reker Daniel; Pfeiffer Bernhard; Altmann Karl-Heinz; Backert Steffen; Wessler Silja; Schneider Gisbert

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Fragment-Based De Novo Design Reveals a Small-Molecule Inhibitor of Helicobacter Pylori HtrA

机译：基于片段的从头设计揭示了幽门螺杆菌HtrA的小分子抑制剂。

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Sustained identification of innovative chemical entities is key for the success of chemical biology and drug discovery. We report the fragment-based, computer-assisted de novo design of a small molecule inhibiting Helicobacter pylori HtrA protease. Molecular binding of the designed compound to HtrA was confirmed through biophysical methods, supporting its functional activity in vitro. Hit expansion led to the identification of the currently best-in-class HtrA inhibitor. The results obtained reinforce the validity of ligand-based de novo design and binding-kinetics-guided optimization for the efficient discovery of pioneering lead structures and prototyping drug-like chemical probes with tailored bioactivity.

机译：持续识别创新化学实体是化学生物学和药物发现成功的关键。我们报告了基于片段的计算机辅助的从头设计的抑制幽门螺杆菌HtrA蛋白酶的小分子。通过生物物理方法证实了所设计化合物与HtrA的分子结合，从而支持了其体外功能活性。命中扩增导致鉴定出目前最佳的HtrA抑制剂。获得的结果加强了基于配体的从头设计和结合动力学指导的优化的有效性，以有效地发现开拓性的先导结构和具有定制生物活性的药物样化学探针的原型。

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《Angewandte Chemie》 |2015年第35期|共5页
作者
Perna Anna M.; Rodrigues Tiago; Schmidt Thomas P.; Boehm Manja; Stutz Katharina; Reker Daniel; Pfeiffer Bernhard; Altmann Karl-Heinz; Backert Steffen; Wessler Silja; Schneider Gisbert;
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biophysical methods; chemical biology; computer-assisted drug design; drug design; receptor-ligand interactions;

机译：生物物理方法;化学生物学;计算机辅助药物设计;药物设计;受体-配体相互作用;

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1. Fragment-Based De Novo Design Reveals a Small-Molecule Inhibitor of Helicobacter Pylori HtrA [J] . Perna Anna M., Rodrigues Tiago, Schmidt Thomas P., Angewandte Chemie . 2015,第35期

机译：基于片段的从头设计揭示了幽门螺杆菌HtrA的小分子抑制剂。
2. Development and characterization of an inducible genetic system in Helicobacter pylori to express a peptide inhibitor of serine protease HtrA [J] . Tegtmeyer N., Boehm M., Backert S. Helicobacter . 2016,第S1期

机译：幽门螺杆菌诱导丝氨酸蛋白酶HtrA肽抑制剂诱导基因系统的开发和鉴定
3. Fragment-based screening identifies inhibitors of ATPase activity and of hexamer formation of Cagα from the Helicobacter pylori type IV secretion system [J] . Tarun Arya, Flore Oudouhou, Bastien Casu, Scientific reports. . 2019,第1期

机译：基于片段的筛选可确定ATP酶活性的抑制剂和来自幽门螺杆菌IV型分泌系统的Cagα六聚体形成的抑制剂
4. Discovering Potent Inhibitors Against the β-Hydroxyacyl-Acyl Carrier Protein Dehydratase (FabZ) of Helicobacter pylori: Structure-Based Design, Synthesis, Bioassay, and Crystal Structure Determination [C] . Lingyan He, Hualiang Jiang, Hong Liu, ICMSI;International conference of molecular simulations and applied informatics technologies . 2010

机译：发现针对幽门螺杆菌的β-羟酰基-酰基载体蛋白脱水酶（FabZ）的有效抑制剂：基于结构的设计，合成，生物测定和晶体结构确定
5. Analysis of mucin oligosaccharides in the rhesus monkey stomach after Helicobacter pylori infection and transcriptional modulation of outer membrane protein expression in Helicobacter pylori [D] . Cooke, Cara Lea 2008

机译：幽门螺杆菌感染后恒河猴胃粘蛋白寡糖分析及幽门螺杆菌外膜蛋白表达的转录调控
6. Fragment-Based De Novo Design Reveals a Small-Molecule Inhibitor ofHelicobacter Pylori HtrA [O] . Dr. Anna M. Perna, Dr. Tiago Rodrigues, Thomas P. Schmidt, -1

机译：基于片段的从头设计揭示了一种小分子抑制剂幽门螺杆菌
7. A novel FRET peptide assay reveals efficient Helicobacter pylori HtrA inhibition through zinc and copper binding [O] . Sabine Bernegger, Cyrill Brunner, Matej Vizovišek, 2020

机译：一种新型的FRET肽测定揭示了通过锌和铜结合的有效幽门螺杆菌HTRA抑制作用

Fragment-Based De Novo Design Reveals a Small-Molecule Inhibitor of Helicobacter Pylori HtrA

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