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Design and synthesis of receptor-selective peptide ligands, and the synthesis of unnatural amino acids.

机译:受体选择性肽配体的设计和合成,以及非天然氨基酸的合成。

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摘要

The discovery of endogenous opioid peptides has greatly accelerated research in opioid chemistry and biology. Studies of the physiological and pharmalogical roles of these receptors require highly potent and receptor-selective ligands for μ, δ, and κ receptors. The major goal of this project is to design and synthesize highly potent and κ receptor-selective dynorphin A analogues with specific conformational and topographical features. Therefore, a series of linear and cyclic dynorphin A analogues with global and/or local conformational constraints have been designed, synthesized, and evaluated for their biological activities. Several leads from dynorphin A analogues have been developed, and have provided new insights into requirements for high κ receptor-selectivity and potency. The incorporation of side chain conformationally constrained amino acids can provide new insights into topographical requirements for peptide ligand-receptor binding. An efficient synthesis of 2', β-dimethyltyrosine in large quantities and a new strategy of the synthesis of optically pure isomers of β-methylphenylalanine derivatives have been developed. These unnatural amino acids can be incorporated into peptides for the development of novel peptides with high potency and enhanced receptor-selectivity.
机译:内源性阿片肽的发现极大地加速了阿片化学和生物学的研究。这些受体的生理和药理作用的研究需要对μ,δ和κ受体具有高度有效的受体选择性配体。该项目的主要目标是设计和合成具有特定构象和地形特征的高效,κ受体选择性强啡肽A类似物。因此,已经设计,合成和评估了具有整体和/或局部构象限制的一系列线性和环状强啡肽A类似物的生物活性。强啡肽A类似物的几条线索已经开发出来,并为高κ受体选择性和效力的要求提供了新的见识。侧链构象受约束的氨基酸的合并可以为肽配体-受体结合的地形要求提供新的见解。已经开发了有效地大量合成2',β-二甲基酪氨酸和合成β-甲基苯基丙氨酸衍生物的光学纯异构体的新策略。可以将这些非天然氨基酸掺入肽中,以开发具有高效力和增强的受体选择性的新型肽。

著录项

  • 作者

    Lung Feng-Di Tiffany.;

  • 作者单位
  • 年度 1995
  • 总页数
  • 原文格式 PDF
  • 正文语种 en
  • 中图分类

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