Texas A&M Drug Discovery Center and Department of Chemistry, College of Arts and Sciences, Texas A&M University, College Station, Texas 77843, United States.
Institute of Biosciences and Technology and Department of Translational Medical Sciences, College of Medicine, Texas A&M University, Houston, Texas 77030, United States.
Chem Rev. 2024 May 8;124(9):6051-6077. doi: 10.1021/acs.chemrev.4c00004. Epub 2024 Apr 30.
Sitting on the interface between biologics and small molecules, peptides represent an emerging class of therapeutics. Numerous techniques have been developed in the past 30 years to take advantage of biological methods to generate and screen peptide libraries for the identification of therapeutic compounds, with phage display being one of the most accessible techniques. Although traditional phage display can generate billions of peptides simultaneously, it is limited to expression of canonical amino acids. Recently, several groups have successfully undergone efforts to apply genetic code expansion to introduce noncanonical amino acids (ncAAs) with novel reactivities and chemistries into phage-displayed peptide libraries. In addition to biological methods, several different chemical approaches have also been used to install noncanonical motifs into phage libraries. This review focuses on these recent advances that have taken advantage of both biological and chemical means for diversification of phage libraries with ncAAs.
坐在生物制剂和小分子之间的界面上,肽代表了一类新兴的治疗药物。在过去的 30 年中,已经开发了许多技术来利用生物方法生成和筛选肽库,以鉴定治疗化合物,其中噬菌体展示是最容易获得的技术之一。尽管传统的噬菌体展示可以同时生成数十亿个肽,但它仅限于表达典型氨基酸。最近,有几个研究小组成功地努力应用遗传密码扩展技术,将具有新颖反应性和化学性质的非典型氨基酸(ncAAs)引入噬菌体展示肽库中。除了生物方法外,还有几种不同的化学方法也被用于将非典型基序安装到噬菌体文库中。这篇综述重点介绍了这些最近的进展,这些进展利用了生物和化学手段,用非典型氨基酸多样化噬菌体文库。
Zotero 插件
