Antimalarial Lead-Optimization Studies on a 2,6-Imidazopyridine Series within a Constrained Chemical Space To Circumvent Atypical Dose-Response Curves against Multidrug Resistant Parasite Strains

Le Manach Claire; Paquet Tanya; Wicht Kathryn; Nchinda Aloysius T.; Brunschwig Christel; Njoroge Mathew; Gibhard Liezl; Taylor Dale; Lawrence Nina; Wittlin Sergio; Eyermann Charles J.; Basarab Gregory S.; Duffy James; Fish Paul V; Street Leslie J.; Chibale Kelly

首页> 外文期刊>Journal of Medicinal Chemistry >Antimalarial Lead-Optimization Studies on a 2,6-Imidazopyridine Series within a Constrained Chemical Space To Circumvent Atypical Dose-Response Curves against Multidrug Resistant Parasite Strains

【24h】

Antimalarial Lead-Optimization Studies on a 2,6-Imidazopyridine Series within a Constrained Chemical Space To Circumvent Atypical Dose-Response Curves against Multidrug Resistant Parasite Strains

机译：在受约束的化学空间内2,6-咪唑嗪的抗疟铅优化研究，以规避非典型剂量 - 反应曲线对多药抗性寄生虫菌株

获取原文

获取原文并翻译 | 示例

获取外文期刊封面封底 >>

开具论文收录证明 >>

文献代查 >>

团队文献服务 >>

页面导航

摘要
著录项
相似文献
相关主题

摘要

A lead-optimization program around a 2,6-imidazopyridine scaffold was initiated based on the two early lead compounds, 1 and 2, that were shown to be efficacious in an in vivo humanized Plasmodium falciparum NODscidIL2R gamma null mouse malaria infection model. The observation of atypical dose-response curves when some compounds were tested against multidrug resistant malaria parasite strains guided the optimization process to define a chemical space that led to typical sigmoidal dose-response and complete kill of multidrug resistant parasites. After a structure and property analysis identified such a chemical space, compounds were prepared that displayed suitable activity, ADME, and safety profiles with respect to cytotoxicity and hERG inhibition.

机译：基于两种早期铅化合物，1和2引发了围绕2,6-咪唑吡啶支架的铅优化程序，其显示在体内人源化疟原虫Nodscividil2R伽马空鼠疟疾感染模型中是有效的。当对多药抗性疟疾测试某些化合物测试某些化合物的非典型剂量 - 反应曲线引导优化过程以定义导致典型的乙状剂量 - 反应并完全杀死多药抗性寄生虫的化学空间。在结构和特性分析确定这种化学空间之后，制备化合物，其相对于细胞毒性和疱疹抑制显示了合适的活性，Adme和安全谱。

著录项

来源
《Journal of Medicinal Chemistry 》 |2018年第20期| 共15页
作者
Le Manach Claire; Paquet Tanya; Wicht Kathryn; Nchinda Aloysius T.; Brunschwig Christel; Njoroge Mathew; Gibhard Liezl; Taylor Dale; Lawrence Nina; Wittlin Sergio; Eyermann Charles J.; Basarab Gregory S.; Duffy James; Fish Paul V; Street Leslie J.; Chibale Kelly;
展开▼
作者单位

Univ Cape Town Drug Discovery &

Dev Ctr H3D Dept Chem ZA-7701 Rondebosch South Africa;

Univ Cape Town Drug Discovery &

Dev Ctr H3D Dept Chem ZA-7701 Rondebosch South Africa;

Univ Cape Town Drug Discovery &

Dev Ctr H3D Dept Chem ZA-7701 Rondebosch South Africa;

Univ Cape Town Drug Discovery &

Dev Ctr H3D Dept Chem ZA-7701 Rondebosch South Africa;

Univ Cape Town Dept Med H3D Div Clin Pharmacol ZA-7925 Observatory South Africa;

Univ Cape Town Dept Med H3D Div Clin Pharmacol ZA-7925 Observatory South Africa;

Univ Cape Town Dept Med H3D Div Clin Pharmacol ZA-7925 Observatory South Africa;

Univ Cape Town Dept Med H3D Div Clin Pharmacol ZA-7925 Observatory South Africa;

Univ Cape Town Dept Med H3D Div Clin Pharmacol ZA-7925 Observatory South Africa;

Swiss Trop &

Publ Hlth Inst Socinstr 57 CH-4002 Basel Switzerland;

Univ Cape Town Drug Discovery &

Dev Ctr H3D Dept Chem ZA-7701 Rondebosch South Africa;

Univ Cape Town Drug Discovery &

Dev Ctr H3D Dept Chem ZA-7701 Rondebosch South Africa;

ICC Med Malaria Venture Route Pre Bois 20 POB 1826 CH-1215 Geneva Switzerland;

UCL UCL Drug Discovery Inst Alzheimers Res UK Cruciform Bldg Gower St London WC1E 6BT England;

Univ Cape Town Drug Discovery &

Dev Ctr H3D Dept Chem ZA-7701 Rondebosch South Africa;

Univ Cape Town Drug Discovery &

Dev Ctr H3D Dept Chem ZA-7701 Rondebosch South Africa;

展开▼
收录信息
原文格式 PDF
正文语种 eng
中图分类药学 ;
关键词

相似文献

外文文献

1. Antimalarial Lead-Optimization Studies on a 2,6-Imidazopyridine Series within a Constrained Chemical Space To Circumvent Atypical Dose-Response Curves against Multidrug Resistant Parasite Strains [J] . Le Manach Claire, Paquet Tanya, Wicht Kathryn, Journal of Medicinal Chemistry . 2018 ,第20期

机译：在受约束的化学空间内2,6-咪唑嗪的抗疟铅优化研究，以规避非典型剂量 - 反应曲线对多药抗性寄生虫菌株
2. Study of the antimalarial activity of 4-aminoquinoline compounds against chloroquine-sensitive and chloroquine-resistant parasite strains [J] . Lawrenson Alexandre S., Cooper David L., ONeill Paul M., Journal of molecular modeling . 2018 ,第9期

机译：4-氨基喹啉化合物对氯喹敏和氯喹抗寄生虫菌株的抗疟活性研究
3. Study of the antimalarial activity of 4-aminoquinoline compounds against chloroquine-sensitive and chloroquine-resistant parasite strains [J] . Alexandre S. Lawrenson, David L. Cooper, Paul M. O’Neill, Journal of molecular modeling . 2018 ,第9期

机译：4-氨基喹啉化合物对氯喹敏和氯喹抗寄生虫菌株的抗疟活性研究
4. Study of the antimalarial activity of 4-aminoquinoline compounds against chloroquine-sensitive and chloroquine-resistant parasite strains [O] . Alexandre S. Lawrenson, David L. Cooper, Paul M. O’Neill, -1

机译：4-氨基喹啉化合物对氯喹敏感性和氯喹抗性寄生虫菌株的抗疟活性研究
5. Antimalarial Lead-Optimization Studies on a 2,6-Imidazopyridine Series within a Constrained Chemical Space To Circumvent Atypical Dose–Response Curves against Multidrug Resistant Parasite Strains [O] . Claire Le Manach, Tanya Paquet, Kathryn Wicht, 2018

机译：在受约束的化学空间内2,6-咪唑嗪的抗疟铅优化研究，以规避非典型剂量 - 反应曲线对多药抗性寄生虫菌株

Antimalarial Lead-Optimization Studies on a 2,6-Imidazopyridine Series within a Constrained Chemical Space To Circumvent Atypical Dose-Response Curves against Multidrug Resistant Parasite Strains

摘要

著录项

相似文献

相关主题

期刊订阅