Backbone-modified amylin derivatives: implications for amyloid inhibitor design and as template for self-assembling bionanomaterials

Elgersma RC; Posthuma G; Rijkers DTS; Liskamp RMJ

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Backbone-modified amylin derivatives: implications for amyloid inhibitor design and as template for self-assembling bionanomaterials

机译：骨干修饰的胰岛淀粉样多肽衍生物：对淀粉样抑制剂设计和自组装仿生纳米材料模板的影响

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This report reviews our approach to the design, synthesis and structural/morphological analysis of backbone-modified amylin(20-29) derivatives. Depending on the position in the peptide backbone and the type of amide bond isostere/modification, the amylin(20-29) peptides behave either as inhibitors of amyloid fibril formation, which are able to retard amyloid formation of native amylin(20-29), or as templates for the formation of self-assembled supramolecular structures. Molecular fine-tuning of the hydrogen-bond accepting/donating properties allows the control over the morphology of the supramolecular aggregation motifs such as helical ribbons and tapes, ribbons progressing to closed peptide nanotubes, (twisted) lamellar sheets or amyloid fibrils. Copyright (c) 2007 European Peptide Society and John Wiley & Sons, Ltd.

机译：这份报告审查了我们的方法设计，合成和骨架/修饰的胰岛淀粉样多肽（20-29）衍生物的结构/形态分析。取决于肽主链上的位置和酰胺键等排体/修饰的类型，淀粉样淀粉样蛋白（20-29）肽可作为淀粉样蛋白原纤维形成的抑制剂，能够抑制天然淀粉样蛋白（20-29）的淀粉样蛋白形成。，或作为形成自组装超分子结构的模板。氢键接受/给予性质的分子微调使得可以控制超分子聚集基序的形态，例如螺旋带和带，带发展成封闭的肽纳米管，（扭曲的）层状薄片或淀粉样原纤维。版权所有（c）2007欧洲多肽协会和John Wiley＆Sons，Ltd.

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《Journal of peptide science: An official publication of the European Peptide Society》 |2007年第11期|共8页
作者
Elgersma RC; Posthuma G; Rijkers DTS; Liskamp RMJ;
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正文语种 eng
中图分类蛋白质的一级结构;
关键词
amyloid; bionanomaterials; helical structures; peptides and peptidomimetics; protein modifications; self-assembly; beta-sheet breaker peptides; supramolecular assemblies; SOLID-PHASE SYNTHESIS; TYPE-2 DIABETES-MELLITUS; FIBRIL FORMATION; BETA-PEPTIDOSULFONAMIDE; PEPTIDE NANOTUBES; BUILDING-BLOCKS; AMINO-ACID; POLYPEPTIDE; AMYLIN(20-29); PROTEIN;

机译：淀粉样蛋白;生物纳米材料;螺旋结构;肽和拟肽;蛋白质修饰;自组装;β-折叠破损肽;超分子组装;固相合成;2型糖尿病-纤维素;纤维形成;BETA-肽二磺酰胺;肽纳米管嵌段;氨基酸;多肽;淀粉蛋白（20-29）;蛋白质;

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1. Backbone-modified amylin derivatives: implications for amyloid inhibitor design and as template for self-assembling bionanomaterials [J] . Elgersma RC, Posthuma G, Rijkers DTS, Journal of peptide science: An official publication of the European Peptide Society . 2007,第11期

机译：骨干修饰的胰岛淀粉样多肽衍生物：对淀粉样抑制剂设计和自组装仿生纳米材料模板的影响
2. Transformation of the amyloidogenic peptide amylin(20-29) into its corresponding peptoid and retropeptoid: access to both an amyloid inhibitor and template for self-assembled supramolecular tapes. [J] . Elgersma RC, Mulder GE, Kruijtzer JA, Bioorganic and Medicinal Chemistry Letters . 2007,第7期

机译：淀粉样蛋白生成肽胰岛淀粉样多肽（20-29）转化为其相应的类肽和类后类肽：获得淀粉样蛋白抑制剂和自组装超分子带的模板。
3. Transformation of the amyloidogenic peptide amylin(20-29) into its corresponding peptoid and retropeptoid: access to both an amyloid inhibitor and template for self-assembled supramolecular tapes. [J] . Elgersma RC, Mulder GE, Kruijtzer JA, Bioorganic and Medicinal Chemistry Letters . 2007,第7期

机译：淀粉样蛋白生成肽胰岛淀粉样多肽（20-29）转化为其相应的类肽和类后类肽：获得淀粉样蛋白抑制剂和自组装超分子带的模板。
4. BACKBONE-MODIFIED AMYLIN DERIVATIVES: IMPLICATIONS FOR AMYLOID INHIBITOR DESIGN AND AS TEMPLATE FOR SELF-ASSEMBLED BIONANOMATERIALS [C] . Ronald C. Elgersma, Dirk T.S. Rijkers, Rob M.J. Liskamp the European Peptide Symposium . 2007

机译：骨架改性淀粉蛋白衍生物：对淀粉样蛋白抑制剂设计的影响和作为自组装小硫代材料的模板
5. Part I: Stucture and dynamics of beta-amyloid fibrils. Part II: Design of Taxol (Paclitaxel) analogs and predictive models; design of measles virus inhibitors; conformational analysis of alpha-helical mimics. [D] . Lakdawala, Ami Sailesh. 2004

机译：第一部分：β-淀粉样蛋白原纤维的结构和动力学。第二部分：紫杉醇（紫杉醇）类似物和预测模型的设计；麻疹病毒抑制剂的设计； α-螺旋模拟物的构象分析。
6. The triphenylmethane dye brilliant blue G is only moderately effective at inhibiting amyloid formation by human amylin or at disaggregating amylin amyloid fibrils, but interferes with amyloid assays; Implications for inhibitor design [O] . Rehana Akter, Alexander Zhyvoloup, Bingqian Zheng, 2012

机译：三苯基甲烷染料亮蓝G仅在抑制人淀粉样蛋白形成淀粉样蛋白或分解淀粉样蛋白淀粉样蛋白原纤维方面具有中等效力，但会干扰淀粉样蛋白的测定。对抑制剂设计的影响
7. The triphenylmethane dye brilliant blue G is only moderately effective at inhibiting amyloid formation by human amylin or at disaggregating amylin amyloid fibrils, but interferes with amyloid assays; Implications for inhibitor design [O] . Rehana Akter, Alexander Zhyvoloup, Bingqian Zheng, 2019

机译：三苯基甲烷染料辉煌的蓝g仅在通过人淀粉蛋白或在分解淀粉蛋白淀粉样淀粉蛋白原纤维中抑制淀粉样蛋白形成，但干扰淀粉样测定;对抑制剂设计的影响

Backbone-modified amylin derivatives: implications for amyloid inhibitor design and as template for self-assembling bionanomaterials

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