Design of novel, potent, noncovalent inhibitors of thrombin with nonbasic P-1 substructures: rapid structure-activity studies by solid-phase synthesis.

Lumma WC Jr; Witherup KM; Tucker TJ; Brady SF; Sisko JT; Naylor-Olsen AM; Lewis SD; Lucas BJ; Vacca JP

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Design of novel, potent, noncovalent inhibitors of thrombin with nonbasic P-1 substructures: rapid structure-activity studies by solid-phase synthesis.

机译：具有非基本P-1亚结构的新型，有效，非共价凝血酶抑制剂的设计：通过固相合成的快速结构活性研究。

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Study of surface representations of the inhibitor-bound thrombin P-1 pocket revealed a lipophilic recess in this pocket which is not occupied by any known inhibitor. Solid-phase synthesis was used to generate benzylamides of D-diphenylAlaPro by aminolysis of Boc dipeptide Kaiser resin. The resulting amides inhibited thrombin in the range IC50 = 3-13,000 nM, and the structure-activity relationships and molecular modeling suggest a unique fit of the benzyl side chain into P-1 with the meta substituent occupying the recess.

机译：研究与抑制剂结合的凝血酶P-1囊袋的表面表示，发现该囊袋中存在亲脂性凹陷，该凹陷不被任何已知的抑制剂占据。通过Boc二肽Kaiser树脂的氨解，使用固相合成生成D-二苯基AlaPro的苄酰胺。所得酰胺在IC50 = 3-13,000 nM范围内抑制凝血酶，并且结构-活性关系和分子模型表明苄基侧链与P-1的独特配合，间位取代基占据了凹槽。

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《Journal of Medicinal Chemistry 》 |1998年第7期| 共3页
作者
Lumma WC Jr; Witherup KM; Tucker TJ; Brady SF; Sisko JT; Naylor-Olsen AM; Lewis SD; Lucas BJ; Vacca JP;
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正文语种 eng
中图分类药学 ;
关键词
Antithrombins; Benzhydryl Compounds; Pyrroles; Thrombin; L-373722; L-377009; 抗凝血酶类; 二苯甲基化合物; 吡咯类; 凝血酶;

机译：Antithrombins;Benzhydryl Compounds;Pyrroles;Thrombin;L-373722;L-377009;抗凝血酶类;二苯甲基化合物;吡咯类;凝血酶;

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1. Design of novel, potent, noncovalent inhibitors of thrombin with nonbasic P-1 substructures: rapid structure-activity studies by solid-phase synthesis. [J] . Lumma WC Jr, Witherup KM, Tucker TJ, Journal of Medicinal Chemistry . 1998 ,第7期

机译：具有非基本P-1亚结构的新型，有效，非共价凝血酶抑制剂的设计：通过固相合成的快速结构活性研究。
2. Design of novel, potent, noncovalent inhibitors of thrombin with nonbasic P-1 substructures: rapid structure-activity studies by solid-phase synthesis. [J] . Lumma WC Jr, Witherup KM, Tucker TJ, Journal of Medicinal Chemistry . 1998 ,第7期

机译：具有非基本P-1亚结构的新型，有效，非共价凝血酶抑制剂的设计：通过固相合成的快速结构活性研究。
3. Design and synthesis of a series of potent and orally bioavailable noncovalent thrombin inhibitors that utilize nonbasic groups in the P1 position. [J] . Tucker TJ, Brady SF, Lumma WC, Journal of Medicinal Chemistry . 1998 ,第17期

机译：设计和合成一系列有效的且口服可生物利用的非共价凝血酶抑制剂，这些抑制剂利用P1位的非碱性基团。
4. Structure-Based Design and Structure-Activity Relationships of D-Phe-Pro-D-Arg-Pr-CONH2 Tetrapeptides Inhibitors of Thrombin [C] . Cristina C. Clement, Manfred Philipp American Peptide Symposium . 2006

机译：基于结构的设计和结构 - 活性关系D-Phe-Pro-D-Arg-Pr-Conh2四肽抑制剂的凝血酶
5. P27 as a molecular target for cancer therapeutics: Discovering small molecule inhibitors of p27 proteolysis and structure-activity relationship and mechanistic studies of largazole, a potent inhibitor of histone deacetylase . [D] . Ungermannova, Dana. 2010

机译：P27作为癌症治疗的分子靶标：发现p27蛋白水解和结构活性关系的小分子抑制剂以及组蛋白脱乙酰基酶的有效抑制剂largazole的机理研究。
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. Molecular recognition at the thrombin active site: structure-based design and synthesis of potent and selective thrombin inhibitors and the X-ray crystal structures of two thrombin-inhibitor complexes [O] . Obst Ulrike, Banner David W., Weber Lutz, 1997

机译：凝血酶活性位点的分子识别：有效和选择性凝血酶抑制剂的结构化设计与合成，以及两种凝血酶抑制剂复合物的X射线晶体结构

Design of novel, potent, noncovalent inhibitors of thrombin with nonbasic P-1 substructures: rapid structure-activity studies by solid-phase synthesis.

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