A novel chemotype of kinase inhibitors: Discovery of 3,4-ring fused 7-azaindoles and deazapurines as potent JAK2 inhibitors.

Wang T; Ledeboer MW; Duffy J

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A novel chemotype of kinase inhibitors: Discovery of 3,4-ring fused 7-azaindoles and deazapurines as potent JAK2 inhibitors.

机译：激酶抑制剂的一种新型趋化型：发现3,4-环融合的7-氮杂胆碱和Deazapurines作为有效的JAK2抑制剂。

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Pictet-Spengler condensation of aldehydes or alpha-keto-esters with 4-(2-anilinophenyl)-7-azaindole (11) or deazapurine (12) gave high yields of the 3,4-fused cyclic compounds. SAR studies, by varying the substituted benzaldehyde components, lead to the discovery of a series of potent JAK2 kinase inhibitors.

机译：用4-（2-苯苯基苯基）-7-氮光（11）或双氮杂环（12）的醛或α-酮酯缩合的醛或α-酮酯缩合，得到了高产3,4稠合环状化合物的产率高。通过改变取代的苯甲醛组分，研究了SAR研究，导致了一系列有效的JAK2激酶抑制剂的发现。

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《Bioorganic and Medicinal Chemistry Letters》 |2010年第1期|共4页
作者
Wang T; Ledeboer MW; Duffy J;
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Vertex Pharmaceuticals Inc. 130 Waverly St. Cambridge MA 02139-4242 United States.;

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正文语种 eng
中图分类药学;生物化学;
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1. A novel chemotype of kinase inhibitors: Discovery of 3,4-ring fused 7-azaindoles and deazapurines as potent JAK2 inhibitors. [J] . Wang T, Ledeboer MW, Duffy J Bioorganic and Medicinal Chemistry Letters . 2010,第1期

机译：激酶抑制剂的一种新型趋化型：发现3,4-环融合的7-氮杂胆碱和Deazapurines作为有效的JAK2抑制剂。
2. Structure-based design of oxygen-linked macrocyclic kinase inhibitors: Discovery of SB1518 and SB1578, potent inhibitors of Janus kinase 2 (JAK2) and Fms-like tyrosine kinase-3 (FLT3) [J] . Poulsen A., William A., Blanchard S., Journal of Computer-Aided Molecular Design . 2012,第4期

机译：基于结构的氧连接大环激酶抑制剂的设计：发现SB1518和SB1578，Janus激酶2（JAK2）和Fms样酪氨酸激酶3（FLT3）的有效抑制剂
3. Structure-based design of oxygen-linked macrocyclic kinase inhibitors: discovery of SB1518 and SB1578, potent inhibitors of Janus kinase 2 (JAK2) and Fms-like tyrosine kinase-3 (FLT3) [J] . Anders Poulsen, Anthony William, Stéphanie Blanchard, Journal of Computer-Aided Molecular Design . 2012,第4期

机译：氧连接大环激酶抑制剂的基于结构的设计：发现SB1518和SB1578，Janus激酶2（JAK2）和Fms样酪氨酸激酶3（FLT3）的有效抑制剂
4. Taking Quinazoline as a General Support-Nog to Design Potent and Selective Kinase Inhibitors: Application to FMS-like Tyrosine Kinase 3 [C] . Wei-Wei Li, Luo-Ding Yu, Li-Juan Chen, ICMSI;International conference of molecular simulations and applied informatics technologies . 2010

机译：以喹唑啉作为一般支持物来设计有效和选择性激酶抑制剂：在类似FMS的酪氨酸激酶3中的应用
5. Biochemical Characterization of FIKK Kinase from Cryptosporidium parvum and Discovery of Potent Inhibitors. [D] . Osman, Khan Tanjid. 2016

机译：小隐隐孢子虫FIKK激酶的生化特征和有效抑制剂的发现。
6. Design and Synthesis of Highly Potent HIV-1 Protease Inhibitors Containing Tricyclic Fused Ring Systems as Novel P2-ligands: Structure-Activity Studies Biological and X-ray Structural Analysis [O] . Arun K. Ghosh, Prasanth R. Nyalapatla, Satish Kovela, -1

机译：包含三环融合环系统作为新型P2-配体的高强度HIV-1蛋白酶抑制剂的设计与合成：结构活性研究生物学和X射线结构分析
7. Germ-line JAK2 mutations in the kinase domain are responsible for hereditary thrombocytosis and are resistant to JAK2 and HSP90 inhibitors. [O] . Marty Caroline, Saint-Martin Cécile, Pecquet Christian, 2014

机译：激酶结构域中的胚系JAK2突变是遗传性血小板增多的原因，并且对JAK2和HSP90抑制剂具有抗性。

A novel chemotype of kinase inhibitors: Discovery of 3,4-ring fused 7-azaindoles and deazapurines as potent JAK2 inhibitors.

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