Engineering another class of anti-tubercular lead: Hit to lead optimization of an intriguing class of gyrase ATPase inhibitors

Jeankumar Variam Ullas; Reshma Rudraraju Srilakshmi; Vats Rahul; Janupally Renuka; Saxena Shalini; Yogeeswari Perumal; Sriram Dharmarajan

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Engineering another class of anti-tubercular lead: Hit to lead optimization of an intriguing class of gyrase ATPase inhibitors

机译：工程化另一类抗结核药的铅：对引人入胜的一类回旋酶ATPase抑制剂进行铅优化

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A structure based medium throughput virtual screening campaign of BITS-Pilani in house chemical library to identify novel binders of Mycobacterium tuberculosis gyrase ATPase domain led to the discovery of a quinoline scaffold. Further medicinal chemistry explorations on the right hand core of the early hit, engendered a potent lead demonstrating superior efficacy both in the enzyme and whole cell screening assay. The binding affinity shown at the enzyme level was further corroborated by biophysical characterization techniques. Early pharmacokinetic evaluation of the optimized analogue was encouraging and provides interesting potential for further optimization. (C) 2016 Elsevier Masson SAS. All rights reserved.

机译：在室内化学文库中基于结构的BITS-Pilani的中等通量虚拟筛选活动，以鉴定结核分枝杆菌回旋酶ATPase结构域的新型结合剂，从而发现了喹啉骨架。在早期打击的右手核心上进行进一步的药物化学探索，产生了强有力的先导，证明了在酶和全细胞筛选测定中均具有优异的功效。通过生物物理表征技术进一步证实了在酶水平上显示的结合亲和力。优化的类似物的早期药代动力学评估令人鼓舞，并为进一步优化提供了有趣的潜力。（C）2016 Elsevier Masson SAS。版权所有。

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《European Journal of Medicinal Chemistry: Chimie Therapeutique》 |2016年第null期|共16页
作者
Jeankumar Variam Ullas; Reshma Rudraraju Srilakshmi; Vats Rahul; Janupally Renuka; Saxena Shalini; Yogeeswari Perumal; Sriram Dharmarajan;
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正文语种 eng
中图分类药学;
关键词
Medium throughput virtual screening; Mycobacterium tuberculosis; DNA gyrase; Differential scanning fluorimetry;

机译：中通量虚拟筛选;结核分枝杆菌;DNA促旋酶;差示扫描荧光法;

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1. Engineering another class of anti-tubercular lead: Hit to lead optimization of an intriguing class of gyrase ATPase inhibitors [J] . Jeankumar Variam Ullas, Reshma Rudraraju Srilakshmi, Vats Rahul, European Journal of Medicinal Chemistry: Chimie Therapeutique . 2016,第Null期

机译：工程化另一类抗结核药的铅：对引人入胜的一类回旋酶ATPase抑制剂进行铅优化
2. Enabling the (3 + 2) cycloaddition reaction in assembling newer anti-tubercular lead acting through the inhibition of the gyrase ATPase domain: lead optimization and structure activity profiling [J] . Variam Ullas Jeankumar, Rudraraju Srilakshmi Reshma, Renuka Janupalty, Organic & biomolecular chemistry . 2015,第8期

机译：通过组装回旋酶ATPase结构域，使（3 + 2）环加成反应能够组装新的抗结核铅：铅优化和结构活性分析
3. Encoded Library Technology as a Source of Hits for the Discovery and Lead Optimization of a Potent and Selective Class of Bactericidal Direct Inhibitors of Mycobacterium tuberculosis InhA [J] . Lourdes Encinas, Heather OKeefe, Margarete Neu, Journal of Medicinal Chemistry . 2014,第4期

机译：编码的图书馆技术可作为发现和潜在优化结核分枝杆菌InhA杀菌有效直接抑制剂的发现和线索优化的命中源
4. Adaptive Lead Weighted ResNet Trained With Different Duration Signals for Classifying 12-lead ECGs [C] . Zhibin Zhao, Hui Fang, Samuel D Relton, Computing in Cardiology . 2020

机译：自适应铅加权reset，具有不同持续时间信号的培训，用于分类12引导ECG
5. Hit-to-Lead” Approaches to Engineering Properties in Conjugated Polymer Semiconductors The alternating copolymer architecture of contemporary π-conjugated polymer semiconductors (PSCs) affords remarkable control over materials properties through combinati [D] . Lopez-Ponnada, Emma V. 2019

机译：命中率“缀合的聚合物半导体中的工程性能方法是当代π缀合的聚合物半导体（PSC）的交替共聚物结构，通过Combinati提供了显着的对材料特性的控制
6. Further validation of strecker-type α-aminonitriles as a new class of potent human carbonic anhydrase II inhibitors: hit expansion within the public domain using differential scanning fluorimetry leads to chemotype refinement [O] . Mikhail Krasavin, Stanislav Kalinin, Sergey Zozulya, 2020

机译：进一步证明strecker型α-氨基腈是新型的有效人类碳酸酐酶II抑制剂：使用差示扫描荧光法在公共领域内的命中扩展导致化学型的完善
7. Encoded library technology as a source of hits for the discovery and lead optimization of a potent and selective class of bactericidal direct inhibitors of mycobacterium tuberculosis inha [O] . Encinas L., OKeefe H., Neu M., 2014

机译：编码文库技术可作为发现和领先优化结核分枝杆菌inha杀菌直接抑制剂有效成分的命中来源

Engineering another class of anti-tubercular lead: Hit to lead optimization of an intriguing class of gyrase ATPase inhibitors

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