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Anchor extension: a structure-guided approach to design cyclic peptides targeting enzyme active sites

机译：锚延伸：设计循环肽靶向酶活性部位的结构引导方法

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摘要

Cyclic peptides are of particular interest due to their pharmacological properties, but their design for binding to a target protein is challenging. Here, the authors present a computational “anchor extension” methodology for de novo design of cyclic peptides that bind to the target protein with high affinity, and validate the approach by developing cyclic peptides that inhibit histone deacetylases 2 and 6.

机译：由于其药理学性质，循环肽特别感兴趣，但它们与靶蛋白结合的设计是挑战性的。这里，作者呈现了一种计算“锚延伸”方法，用于与具有高亲和力结合的环状肽的循环肽的Novo设计，并通过开发抑制组蛋白脱乙酰酶2和6的环状肽来验证方法。

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作者
Parisa Hosseinzadeh; Paris R. Watson; Timothy W. Craven; Xinting Li; Stephen Rettie; Fátima Pardo-Avila; Asim K. Bera; Vikram Khipple Mulligan; Peilong Lu; Alexander S. Ford; Brian D. Weitzner; Lance J. Stewart; Adam P. Moyer; Maddalena Di Piazza; Joshua G. Whalen; Per Greisen; David W. Christianson; David Baker;
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年度 2021
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正文语种 eng
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专利

1. Structure-Guided Design, Synthesis, and Evaluation of Salicylic Acid-Based Inhibitors Targeting a Selectivity Pocket in the Active Site of Human 20 alpha-Hydroxysteroid Dehydrogenase (AKR1C1) [J] . El-Kabbani O, Scammells PJ, Gosling J, Journal of Medicinal Chemistry . 2009,第10期

机译：基于水杨酸的抑制剂在人20α-羟基类固醇脱氢酶（AKR1C1）活性位点的结构导向设计，合成和评估
2. Discovery of cyclic sulfoxide hydroxyethylamines as potent and selective β-site APP-cleaving enzyme 1 (BACE1) inhibitors: Structure based design and in vivo reduction of amyloid β-peptides [J] . RueegerH., LueoendR., MachauerR., Bioorganic and Medicinal Chemistry Letters . 2013,第19期

机译：发现环状亚砜羟乙胺作为有效的选择性β-位APP裂解酶1（BACE1）抑制剂：基于结构的设计和淀粉样β肽的体内还原
3. Discovery of cyclic sulfone hydroxyethylamines as potent and selective β-site APP-cleaving enzyme 1 (BACE1) inhibitors: Structure-based design and in vivo reduction of amyloid β-peptides [J] . Rueeger H., Lueoend R., Rogel O., Journal of Medicinal Chemistry . 2012,第7期

机译：发现环状砜羟乙胺作为有效的选择性β-位APP裂解酶1（BACE1）抑制剂：基于结构的设计和淀粉样β肽的体内还原
4. SECONDARY STRUCTURE ANALYSIS OF TWO RECOMBINANT PEPTIDES FROM ACTIVE SITES OF HUMAN ANGIOTENSIN CONVERTING ENZYME (ACE) [C] . Sotirios Spyridon M. Vamvakas, Leondios Leondiadis, Georgios A. Spyroulias the European Peptide Symposium . 2007

机译：两种重组肽的二次结构分析，来自人血管紧张素转化酶的活性位点（ACE）
5. Structure-Guided Design and Synthesis of Small Molecules Targeting Hepatitis C Virus Internal Ribosome Entry Site RNA. [D] . Ding, Kejia. 2014

机译：针对丙型肝炎病毒内部核糖体进入位点RNA的小分子的结构指导设计和合成。
6. Design of peptide enzymes (pepzymes): surface-simulation synthetic peptides that mimic the chymotrypsin and trypsin active sites exhibit the activity and specificity of the respective enzyme. [O] . M Z Atassi, T Manshouri 1993

机译：肽酶（pepzymes）的设计：模拟胰凝乳蛋白酶和胰蛋白酶活性位点的表面模拟合成肽表现出相应酶的活性和特异性。
7. Design of peptide enzymes (pepzymes): surface-simulation synthetic peptides that mimic the chymotrypsin and trypsin active sites exhibit the activity and specificity of the respective enzyme. [O] . Atassi, M Z, Manshouri, T 1993

机译：肽酶（pepzymes）的设计：模仿糜蛋白酶和胰蛋白酶活性位点的表面模拟合成肽表现出相应酶的活性和特异性。

Anchor extension: a structure-guided approach to design cyclic peptides targeting enzyme active sites

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