Hayward Deanne, Beekman Andrew M
School of Pharmacy, University of East Anglia, Norwich Research Park Norwich Norfolk NR47TJ UK
RSC Chem Biol. 2024 Feb 16;5(3):198-208. doi: 10.1039/d3cb00222e. eCollection 2024 Mar 6.
The development of small molecules that interact with protein-protein interactions is an ongoing challenge. Peptides offer a starting point in the drug discovery process for targeting protein-interactions due to their larger, more flexible structure and the structurally diverse properties that allow for a greater interaction with the protein. The techniques for rapidly identifying potent cyclic peptides and turn-motif peptides are highly effective, but this potential has not yet transferred to approved drug candidates. By applying the properties of the peptide-protein interaction the development of small molecules for drug discovery has the potential to be more efficient. In this review, we discuss the methods that allow for the unique binding properties of peptides to proteins, and the methods deployed to transfer these qualities to potent small molecules.
开发能与蛋白质-蛋白质相互作用的小分子仍是一项持续的挑战。由于肽具有更大、更灵活的结构以及能与蛋白质产生更强相互作用的多样结构特性,因此在药物发现过程中,肽为靶向蛋白质相互作用提供了一个起点。快速鉴定强效环肽和转角基序肽的技术非常有效,但这种潜力尚未转化为获批的候选药物。通过应用肽-蛋白质相互作用的特性,开发用于药物发现的小分子有可能更高效。在本综述中,我们讨论了能够实现肽与蛋白质独特结合特性的方法,以及用于将这些特性转化为强效小分子的方法。
