Discovery of Novel P1 Groups for Coagulation Factor VIIa Inhibition Using Fragment-Based Screening

Cheney Daniel L.; Bozarth Jeffrey M.; Metzler William J.; Morin Paul E.; Mueller Luciano; Newitt John A.; Nirschl Alexandra H.; Rendina Alan R.; Tamura James K.; Wei Anzhi; Wen Xiao; Wurtz Nicholas R.; Seiffert Dietmar A.; Wexler Ruth R.; Priestley E. Scott

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Discovery of Novel P1 Groups for Coagulation Factor VIIa Inhibition Using Fragment-Based Screening

机译：发现新的P1组凝血因子VIIa抑制使用基于片段的筛选。

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A multidisciplinary, fragment-based screening approach involving protein ensemble docking and biochemical and NMR assays is described. This approach led to the discovery of several structurally diverse, neutral surrogates for cationic factor VIIa P1 groups, which are generally associated with poor pharmacokinetic (PK) properties. Among the novel factor VIIa inhibitory fragments identified were aryl halides, lactams, and heterocycles. Crystallographic structures for several bound fragments were obtained, leading to the successful design of a potent factor Vila inhibitor with a neutral lactam PI and improved permeability.

机译：描述了一种多学科，基于片段的筛选方法，涉及蛋白质整体对接以及生化和NMR分析。这种方法导致发现了几种结构上不同的阳离子因子VIIa P1基团的中性替代物，这些替代物通常与不良的药代动力学（PK）性能有关。在新发现的VIIa因子抑制性片段中，有芳基卤化物，内酰胺和杂环。获得了几个结合片段的晶体结构，从而成功设计了具有中性内酰胺PI和改善的通透性的有效因子Vila抑制剂。

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《Journal of Medicinal Chemistry》 |2015年第6期|共10页
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Cheney Daniel L.; Bozarth Jeffrey M.; Metzler William J.; Morin Paul E.; Mueller Luciano; Newitt John A.; Nirschl Alexandra H.; Rendina Alan R.; Tamura James K.; Wei Anzhi; Wen Xiao; Wurtz Nicholas R.; Seiffert Dietmar A.; Wexler Ruth R.; Priestley E. Scott;
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1. Discovery of Novel P1 Groups for Coagulation Factor VIIa Inhibition Using Fragment-Based Screening [J] . Cheney Daniel L., Bozarth Jeffrey M., Metzler William J., Journal of Medicinal Chemistry . 2015,第6期

机译：发现新的P1组凝血因子VIIa抑制使用基于片段的筛选。
2. More efficient reversal of dabigatran inhibition of coagulation by activated prothrombin complex concentrate or recombinant factor VIIa than by four-factor prothrombin complex concentrate [J] . Lindahl Tomas L., Wallstedt Maria, Gustafsson Kerstin M., Thrombosis Research: An International Journal on Vascular Obstruction, Hemorrhage and Hemostasis . 2015,第3期

机译：活化的凝血酶原复合物浓缩物或重组凝血因子VIIa比四因子凝血酶原复合物浓缩物更有效地逆转达比加群抑制凝血的作用
3. Ancylostoma ceylanicum anticoagulant peptide-1: role of the predicted reactive site amino acid in mediating inhibition of coagulation factors Xa and VIIa. [J] . Mieszczanek J, Harrison LM, Cappello M Molecular and Biochemical Parasitology . 2004,第1期

机译：鞘氨醇单胞菌抗凝血肽-1：预测的反应位点氨基酸在介导凝血因子Xa和VIIa抑制中的作用。
4. FACTOR VIIA INHIBITION BY NATURALLY OCCURRING PEAT HUMIC ACIDS AND SYNTHETIC HUMIC ACID LIKE POLYMERS [C] . Hans-Peter Kloecking, NICOLLE Mahr, Karl Heinz Heise, International Peat Congress; 20040606-11; Tampere(FI) . 2004

机译：天然产生的腐殖酸和类似腐殖酸的聚合物对因子的抑制作用
5. Validating dynamic pharmacophore based virtual screening and *computational insight into human blood coagulation factor Xa subsites [D] . Singh, Narender 2007

机译：验证基于动态药效团的虚拟筛选和*对人类凝血因子Xa子位点的计算洞察力
6. First epidermal growth factor-like domain of human blood coagulation factor IX is required for its activation by factor VIIa/tissue factor but not by factor XIa. [O] . D Zhong, K J Smith, J J Birktoft, 1994

机译：人凝血因子IX的第一个表皮生长因子样结构域是通过因子VIIa /组织因子而不是因子XIa激活所必需的。
7. More efficient reversal of dabigatran inhibition of coagulation by activated prothrombin complex concentrate or recombinant factor VIIa than by four-factor prothrombin complex concentrate [O] . Lindahl, Tomas, Wallstedt, Maria, Gustafsson, Kerstin, 2015

机译：活化的凝血酶原复合物浓缩物或重组因子VIIa比四因子凝血酶原复合物浓缩物更有效地逆转达比加群抑制凝血的作用

Discovery of Novel P1 Groups for Coagulation Factor VIIa Inhibition Using Fragment-Based Screening

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