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Impact of Hydrogen-Bond Surrogate Model on Helix Stabilization and Development of Protein-Protein Interaction Inhibitors

机译:氢键替代模型对螺旋稳定和蛋白质-蛋白质相互作用抑制剂发展的影响

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摘要

Protein-protein interactions (PPIs) involved in several diseases are predominantly mediated through short helical peptides. Unlike small molecules, due to the extended surface, the chemically constrained peptides with proper helical conformation can modulate the PPIs and thus contribute to the future drug developments. Several model systems have been introduced in the past to induce the helical structure in short peptides. Incorporating the unnatural constraints by various protocols has been excellent in biasing helical conformation and improving the proteolytic stability and the cell permeability of peptides. Hydrogen-bond surrogate (HBS) is one of such well-known protocols to mimic helical surfaces in numerous peptide sequences. Unlike ‘Stapled’ peptides, HBSmodel replaces the main-chain i+4!i hydrogen bonding interaction with a covalent surrogate and retains the side-chain functionality intact, which is beneficial for targeting multi-faced PPIs. This review focuses on the chemistry behind the development of the HBS-stabilized peptides, its biophysical characterizations, and numerous biological applications. Furthermore, this review will provide a broad overview of the HBS-model to attract chemical biologists to target multifaced ‘difficult’ PPIs.
机译:蛋白质-蛋白质之间的关系(质子泵抑制剂)参与几个主要是介导的疾病通过短螺旋肽。分子,由于表面,延长化学肽通过适当的限制螺旋构象可以调节质子泵抑制剂从而为未来药物发展作出贡献。介绍了几种模型系统过去的诱导短的螺旋结构肽。通过各种协议的偏置螺旋构象和改善蛋白水解稳定性和细胞通透性肽。这样的知名协议模拟螺旋表面在众多肽序列。“钉”肽,HBSmodel取代了主链我+ 4 !共价代理人和保留侧链功能完整,这是有利于目标多边形质子泵抑制剂。回顾关注背后的化学发展HBS-stabilized肽,它生物物理特征,众多生物应用。将提供一个广泛的概述HBS-model吸引目标multifaced化学生物学家‘difficult’PPIs)。

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  • 来源
    《Chemistry Select》 |2023年第10期|1-11|共11页
  • 作者

    Sunit Pal;

  • 作者单位

    Chemical Genomics Centre of the Max Planck Society Max Planck Institute of Molecular Physiology Otto-Hahn-Str. 11, 44227 Dortmund Germany;

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  • 正文语种 英语
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