A Molecular Hybridization Approach for the Design of Potent, Highly Selective, and Brain-Penetrant N-Myristoyltransferase Inhibitors

Harrison Justin R.; Brand Stephen; Smith Victoria; Robinson David A.; Thompson Stephen; Smith Alasdair; Davies Kenneth; Mok Ngai; Torrie Leah S.; Collie Iain; Hallyburton Irene; Norval Suzanne; Simeons Frederick R. C.; Stojanovski Laste; Frearson Julie A.; Brenk Ruth; Wyatt Paul G.; Gilbert Ian H.; Read Kevin D.

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A Molecular Hybridization Approach for the Design of Potent, Highly Selective, and Brain-Penetrant N-Myristoyltransferase Inhibitors

机译：用于设计有效，高选择性和脑渗透N-Myristoyltransfase酶抑制剂的分子杂交方法

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Crystallography has guided the hybridization of two series of Trypanosoma brucei N-myristoyltransferase (NMT) inhibitors, leading to a novel highly selective series. The effect of combining the selectivity enhancing elements from two pharmacophores is shown to be additive and has led to compounds that have greater than 1000-fold selectivity for TbNMT vs HsNMT. Further optimization of the hybrid series has identified compounds with significant trypanocidal activity capable of crossing the blood-brain barrier. By using CF-1 mdr1a deficient mice, we were able to demonstrate full cures in vivo in a mouse model of stage 2 African sleeping sickness. This and previous work provides very strong validation for NMT as a drug target for human African trypanosomiasis in both the peripheral and central nervous system stages of disease.

机译：晶体学引导了两系列触发瘤斑米菌霉菌直流酶（NMT）抑制剂的杂交，导致新颖的高度选择性系列。组合来自两种药物团的选择性增强元件的效果被显示为添加剂，并导致具有大于1000倍的Tbnmt与HsnMT的选择性的化合物。杂交系的进一步优化已鉴定具有能够穿过血脑屏障的显着胰蛋白酶活性的化合物。通过使用CF-1MDR1A缺陷小鼠，我们能够在阶段2阶段非洲睡眠疾病的小鼠模型中展示体内的全部治疗。此前和以前的工作为NMT作为疾病的外周和中枢神经系统阶段中的人类非洲锥虫病毒的药物目标提供了非常强烈的验证。

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《Journal of Medicinal Chemistry 》 |2018年第18期| 共16页
作者
Harrison Justin R.; Brand Stephen; Smith Victoria; Robinson David A.; Thompson Stephen; Smith Alasdair; Davies Kenneth; Mok Ngai; Torrie Leah S.; Collie Iain; Hallyburton Irene; Norval Suzanne; Simeons Frederick R. C.; Stojanovski Laste; Frearson Julie A.; Brenk Ruth; Wyatt Paul G.; Gilbert Ian H.; Read Kevin D.;
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作者单位

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

Univ Dundee Wellcome Ctr Antiinfect Res Sch Life Sci Div Biol Chem &

Drug Discovery Drug Discovery Uni Dundee Scotland;

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1. A Molecular Hybridization Approach for the Design of Potent, Highly Selective, and Brain-Penetrant N-Myristoyltransferase Inhibitors [J] . Harrison Justin R., Brand Stephen, Smith Victoria, Journal of Medicinal Chemistry . 2018 ,第18期

机译：用于设计有效，高选择性和脑渗透N-Myristoyltransfase酶抑制剂的分子杂交方法
2. Design and synthesis of a novel 2-oxindole scaffold as a highly potent and brain-penetrant phosphodiesterase 10A inhibitor [J] . Yoshikawa Masato, Kamisaki Haruhi, Kunitomo Jun, Bioorganic and medicinal chemistry . 2015 ,第22期

机译：设计和合成新型2-氧吲哚支架作为高效和脑渗透性磷酸二酯酶10A抑制剂
3. Type IIA - Type IIB protein tyrosine kinase inhibitors hybridization as an efficient approach for potent multikinase inhibitor development: Design, synthesis, anti-proliferative activity, multikinase inhibitory activity and molecular modeling of novel indolinone-based ureides and amides [J] . Eldehna Wagdy M., El Kerdawy Ahmed M., Al-Ansary Ghada H., European Journal of Medicinal Chemistry: Chimie Therapeutique . 2019 ,第期

机译：IIA型IIB型IIB蛋白酪氨酸激酶抑制剂杂交作为有效的多立糖酶抑制剂显影的有效方法：设计，合成，抗增殖活性，多喹啉基脲和酰胺的新型吲哚酮的硫化物和酰胺的分子建模
4. PROTEIN EPITOPE MIMETICS: AN INNOVATIVE APPROACH TO THE DISCOVERY OF SELECTIVE AND HIGHLY POTENT SERINE PROTEASE INHIBITORS [C] . Odile Sellier, Francoise Jung, Steve J. DeMarco the European Peptide Symposium . 2007

机译：蛋白表位模拟方法：一种创新的选择性和高效丝氨酸蛋白酶抑制剂的方法
5. Towards the design of highly selective molecularly imprinted hydrogels for biosensor applications. [D] . Padro Cortes, Lorena R. 2009

机译：致力于生物传感器应用的高选择性分子印迹水凝胶的设计。
6. A Molecular HybridizationApproach for the Designof Potent Highly Selective and Brain-Penetrant N-Myristoyltransferase Inhibitors [O] . JustinR. Harrison, Stephen Brand, Victoria Smith, -1

机译：分子杂交设计方法强效高选择性和脑渗透性N-肉豆蔻酰转移酶抑制剂的合成
7. A Molecular Hybridization Approach for the Design of Potent, Highly Selective, and Brain-Penetrant N-Myristoyltransferase Inhibitors [O] . Justin R. Harrison, Stephen Brand, Victoria Smith, 2018

机译：用于设计有效，高选择性和脑渗透N-Myristoyltransfase酶抑制剂的分子杂交方法

A Molecular Hybridization Approach for the Design of Potent, Highly Selective, and Brain-Penetrant N-Myristoyltransferase Inhibitors

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