Zhang Yanyan, Zhou Shanggen, Wavreille Anne-Sophie, DeWille James, Pei Dehua
Department of Chemistry and Ohio State Biochemistry Program, The Ohio State University, 100 West 18th Avenue, Columbus, Ohio 43210, USA.
J Comb Chem. 2008 Mar-Apr;10(2):247-55. doi: 10.1021/cc700185g. Epub 2008 Feb 8.
Cyclic peptides provide attractive lead compounds for drug discovery and excellent molecular probes in biomedical research. In this work, a novel method has been developed for the high-throughput synthesis, screening, and identification of cyclic peptidyl ligands against macromolecular targets. Support-bound cyclic phosphotyrosyl peptide libraries containing randomized amino acid sequences and different ring sizes (theoretical diversity of 3.2 x 10(6)) were synthesized and screened against the SH2 domains of Grb2 and tensin. Potent, selective inhibitors were identified from the libraries and were generally more effective than the corresponding linear peptides. One of the inhibitors selected against the Grb2 SH2 domain inhibited human breast cancer cell growth and disrupted actin filaments. This method should be applicable to the development of cyclic peptidyl inhibitors against other protein domains, enzymes, and receptors.
环肽为药物研发提供了有吸引力的先导化合物,也是生物医学研究中出色的分子探针。在这项工作中,已开发出一种新方法,用于针对大分子靶标的环肽基配体的高通量合成、筛选和鉴定。合成了支持物结合的环磷酸酪氨酸肽库,其包含随机化的氨基酸序列和不同的环大小(理论多样性为3.2×10⁶),并针对Grb2和张力蛋白的SH2结构域进行筛选。从库中鉴定出了强效、选择性抑制剂,且它们通常比相应的线性肽更有效。针对Grb2 SH2结构域选择的一种抑制剂可抑制人乳腺癌细胞生长并破坏肌动蛋白丝。该方法应适用于开发针对其他蛋白质结构域、酶和受体的环肽基抑制剂。
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