Structure-Based Design of Irreversible Human KAT II Inhibitors: Discovery of New Potency-Enhancing Interactions

Jamison B. Tuttle; Marie Anderson; Bruce M. Bechle

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Structure-Based Design of Irreversible Human KAT II Inhibitors: Discovery of New Potency-Enhancing Interactions

机译：基于结构的不可逆人类KAT II抑制剂的设计：发现新的增强效能的相互作用。

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A series of aryl hydroxamates recently have been disclosed as irreversible inhibitors of kynurenine amino transferase II (KAT II), an enzyme that may play a role in schizophrenia and other psychiatric and neurological disorders. The utilization of structure?activity relationships (SAR) in conjunction with X-ray crystallography led to the discovery of hydroxamate 4, a disubstituted analogue that has a significant potency enhancement due to a novel interaction with KAT II. The use of k_(inact)/K_i to assess potency was critical for understanding the SAR in this series and for identifying compounds with improved pharmacodynamic profiles.

机译：最近已公开了一系列芳基异羟肟酸酯作为犬尿氨酸氨基转移酶II（KAT II）的不可逆抑制剂，该酶可能在精神分裂症和其他精神病和神经疾病中起作用。与X射线晶体学结合使用结构活性关系（SAR）导致发现了异羟肟酸酯4，它是一种双取代的类似物，由于与KAT II发生了新的相互作用而具有显着的效能增强。使用k_（inact）/ K_i评估效力对于理解本系列中的SAR和鉴定具有改善的药效学特征的化合物至关重要。

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《ACS medicinal chemistry letters》 |2013年第1期|共4页
作者
Jamison B. Tuttle; Marie Anderson; Bruce M. Bechle;
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正文语种 eng
中图分类药学;
关键词
kynurenine amino transferase; kynurenic acid; aryl hydrocarbon receptor; irreversible inhibition; hydroxamic acid; dose response modeling; in vivo microdialysis; schizophrenia;

机译：犬尿氨酸氨基转移酶;犬尿酸;芳烃受体;不可逆抑制;异羟肟酸;剂量反应模型;体内微透析;精神分裂症;

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1. Structure-Based Design of Irreversible Human KAT II Inhibitors: Discovery of New Potency-Enhancing Interactions [J] . Jamison B. Tuttle, Marie Anderson, Bruce M. Bechle ACS medicinal chemistry letters . 2013,第1期

机译：基于结构的不可逆人类KAT II抑制剂的设计：发现新的增强效能的相互作用。
2. Structure-Based Design of a Parallel Synthetic Array Directed Toward the Discovery of Irreversible Inhibitors of Human Rhinovirus 3C Protease [J] . Theodore O. Johnson, Ye Hua, Hiep T. Luu, Journal of Medicinal Chemistry . 2002,第10期

机译：针对人类鼻病毒3C蛋白酶不可逆抑制剂发现的并行合成阵列的基于结构的设计。
3. Discovery of N-((3R,4R)-4-Fluoro-1-(6-((3-methoxy-1-methyl-1H-pyrazol-4-yl)amino)-9-methyl-9H-purin-2-yl)pyrrolidine-3-yl)acrylamide (PF-06747775) through Structure-Based Drug Design: A High Affinity Irreversible Inhibitor Targeting Oncogenic EGFR Mutants with Selectivity over Wild-Type EGFR [J] . Planken Simon, Behenna Douglas C., Nair Sajiv K., Journal of Medicinal Chemistry . 2017,第7期

机译：发现N - （（3R，4R）-4-氟-1-（6 - （（3-甲氧基-1-甲基-1H-吡唑-4-基）氨基）-9-甲基-9H-五林-2 - 吡咯烷-3-基）丙烯酰胺（PF-06747775）通过基于结构的药物设计：一种高亲和力不可逆抑制剂，靶向癌症EGFR突变体，在野生型EGFR上选择性
4. Inactiwatlon of Animal Factor VIII by human Factor VIII Inhibitors: Inwestigation of Plasma from Patients with Inhibitors in congenital Hemophilia I and from Patients with acquired Hemophilia A [C] . V. Aumann, G. Lutze (Jr.), G. Lutze (Sen.), Hemophilie-Symposion . 2003

机译：人为因子VIII抑制剂的动物因子VIII的乙酰丁酮：先天性血友病药中抑制剂患者的血浆中的预防
5. Structure-based design and discovery of small molecule inhibitors of protein-protein interactions. [D] . Lu, Yipin. 2006

机译：基于结构的设计和蛋白质-蛋白质相互作用的小分子抑制剂的发现。
6. Structure-Based Designof Irreversible Human KAT II Inhibitors: Discovery of New Potency-EnhancingInteractions [O] . Jamison B. Tuttle, *, †, 2013

机译：基于结构的设计不可逆的人类KAT II抑制剂的研究：新的增强功效的发现互动互动
7. Structure-Based Design of Irreversible Human KAT II Inhibitors: Discovery of New Potency-Enhancing Interactions [O] . Jamison B. Tuttle, Marie Anderson, Bruce M. Bechle, 2012

机译：不可逆人KAT II抑制剂的基于结构的设计：发现新的效力增强互动

Structure-Based Design of Irreversible Human KAT II Inhibitors: Discovery of New Potency-Enhancing Interactions

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