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首页> 外文期刊>Current Medicinal Chemistry >Recent Development of Cyclic Amide (Pyridone/Lactam) Moiety Containing Heterocycles as Protein Kinase Inhibitors
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Recent Development of Cyclic Amide (Pyridone/Lactam) Moiety Containing Heterocycles as Protein Kinase Inhibitors

机译:含杂环的环酰胺(吡啶酮/内酰胺)部分作为蛋白激酶抑制剂的最新进展

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摘要

Staurosporine, pyridone 6 and hydroxyfasudil are cyclic amide (pyridone/lactam) moiety containing heterocycles that are discovered/developed as potent protein kinase inhibitors targeting on the ATP (Adenosine-5'-triphosphate) binding pocket. Despite different molecular shapes (pentacycle, tetracycle and bicycle, respectively), they all bind to the residues of the hinge region at ATP binding pocket of protein kinases in a very similar manner: the cyclic amide moiety occupies the adenine region of ATP binding pocket and forms at least two hydrogen bonding interaction with the hinge region via its hydrogen bond acceptor/donor pair. Using a few examples of cyclic amide (pyridone/lactam) moiety containing heterocyclic protein kinase inhibitors, this review discusses their therapeutic application, structural basis of kinase inhibition, as well as their associated syntheses. It is anticipated that the design, synthesis and profiling of the kinasebiased library based upon the cyclic amide (pyridone/lactam) moiety containing core scaffolds may significantly enhance the efficiency of high-throughput screenings (HTS), accelerate hit-to-lead process and improve the success rate in the development of protein kinase inhibitors for the treatment of various diseases especially cancer.
机译:星形孢菌素,吡啶酮6和羟基法舒地尔是含有杂环的环状酰胺(吡啶酮/内酰胺)部分,已被发现/开发为靶向ATP(腺苷5'-三磷酸)结合口袋的有效蛋白激酶抑制剂。尽管分子形状不同(分别为五环,四环和自行车),它们都以非常相似的方式结合至蛋白激酶ATP结合口袋的铰链区残基:环酰胺部分占据ATP结合口袋的腺嘌呤区,而经由其氢键受体/供体对与铰链区形成至少两个氢键相互作用。本文使用含有杂环蛋白激酶抑制剂的环状酰胺(吡啶酮/内酰胺)部分的一些实例,讨论了它们的治疗应用,激酶抑制的结构基础以及相关的合成方法。预期基于包含核心骨架的环状酰胺(吡啶酮/内酰胺)部分的激酶偏倚文库的设计,合成和分析可以显着提高高通量筛选(HTS)的效率,加速从头到尾的流程和提高了开发用于各种疾病(尤其是癌症)的蛋白激酶抑制剂的成功率。

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