Structure-Based Design of Macrocyclic Coagulation Factor Vila Inhibitors

Priestley E. Scott; Cheney Daniel L.; DeLucca Indawati; Wei Anzhi; Luettgen Joseph M.; Rendina Alan R.; Wong Pancras C.; Wexler Ruth R.

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Structure-Based Design of Macrocyclic Coagulation Factor Vila Inhibitors

机译：大环凝血因子VIIa抑制剂的基于结构的设计

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On the basis of a crystal structure of a phenylpyrrolidine lead and subsequent molecular modeling results, we designed and synthesized a novel series of macrocyclic FVlIa inhibitors. The optimal 16-membered macrocyde was 60-fold more potent than an acyclic analog. Further potency optimization by incorporation of P1' alkyl sulfone and P2 methyl groups provided a macrocyde with TF/FVIIa K-i = 1.6 nM, excellent selectivity against a panel of seven serine proteases, and FVII-deficient prothrombin time EC2x = 1.2 mu M. Discovery of this potent, selective macrocyclic scaffold opens new possibilities for the development of orally bioavailable FVIIa inhibitors.

机译：基于苯基吡咯烷铅的晶体结构和随后的分子建模结果，我们设计和合成了一系列新的大环FV11a抑制剂。最佳的16元大环比无环类似物的效价高60倍。通过并入P1'烷基砜和P2甲基进一步优化效能，提供了一个大环，其TF / FVIIa Ki = 1.6 nM，对一组七种丝氨酸蛋白酶的优异选择性，以及FVII缺乏的凝血酶原时间EC2x = 1.2μM。这种有效的，选择性的大环支架为口服生物利用性FVIIa抑制剂的开发开辟了新的可能性。

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《Journal of Medicinal Chemistry 》 |2015年第15期| 共12页
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Priestley E. Scott; Cheney Daniel L.; DeLucca Indawati; Wei Anzhi; Luettgen Joseph M.; Rendina Alan R.; Wong Pancras C.; Wexler Ruth R.;
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1. Structure-Based Design of Macrocyclic Coagulation Factor Vila Inhibitors [J] . Priestley E. Scott, Cheney Daniel L., DeLucca Indawati, Journal of Medicinal Chemistry . 2015 ,第15期

机译：大环凝血因子VIIa抑制剂的基于结构的设计
2. Structure-based design of nitrogen-linked macrocyclic kinase inhibitors leading to the clinical candidate SB1317/TG02, a potent inhibitor of cyclin dependant kinases (CDKs), Janus kinase 2 (JAK2), and Fms-like tyrosine kinase-3 (FLT3) [J] . Poulsen A., William A., Blanchard S., Journal of molecular modeling . 2013 ,第1期

机译：基于结构的氮连接大环激酶抑制剂的设计导致临床候选药物SB1317 / TG02，这是细胞周期蛋白依赖性激酶（CDK），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] . 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
4. Binding of Coagulation Factor Vila to Cell Surface Tissue Factor Induces Signal Transduction via p44/p42MAPK [C] . B.B. Sorensen. L.K. Poulsen, M. Ezban, L.C. Petersen NATO Advanced Study Institute on Vascular Endothelium : Mechanisms of Cell Signaling . 1999

机译：凝血因子VILA与细胞表面组织因子的结合通过P44 / P42MAPK引起信号转导
5. Design of Novel Inhibitors for Infectious Diseases using Structure-based Drug Design: Virtual Screening, Homology Modeling and Molecular Dynamics. [D] . Ramamoorthy, Divya. 2012

机译：使用基于结构的药物设计设计新型传染病抑制剂：虚拟筛选，同源性建模和分子动力学。
6. Structure-Based Design and Synthesis of Triazole-based Macrocyclic Inhibitors of Norovirus Protease: Structural Biochemical Spectroscopic and Antiviral Studies [O] . Pathum M. Weerawarna, Yunjeong Kim, Anushka C. Galasiti Kankanamalage, -1

机译：基于三唑的诺如病毒蛋白酶大环抑制剂的结构设计与合成：结构生化光谱和抗病毒研究
7. Design and Synthesis of Depeptidized Macrocyclic Inhibitors of Hepatitis C NS3-4A Protease Using Structure-Based Drug Design [O] . -1

机译：基于结构的药物设计的丙型肝炎蛋白酶缺陷大环抑制剂的设计与合成

Structure-Based Design of Macrocyclic Coagulation Factor Vila Inhibitors

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