Department of Chemistry, Graduate School of Science, The University of Tokyo, Tokyo, Japan.
Department of Biochemistry, Graduate School of Medicine, Yokohama City University, Yokohama, Japan.
Nat Chem. 2020 Nov;12(11):1081-1088. doi: 10.1038/s41557-020-0525-1. Epub 2020 Aug 24.
Peptides that contain β-amino acids display stable secondary structures, such as helices and sheets, and are often referred to as foldamers. Cyclic β-amino acids (cβAAs), such as 2-aminocyclohexanecarboxylic acid (2-ACHC), are strong helix/turn inducers due to their restricted conformations. Here we report the ribosomal synthesis of foldamer peptides that contain multiple, up to ten, consecutive cβAAs via genetic code reprogramming. We also report the de novo discovery of macrocyclic cβAA-containing peptides capable of binding to a protein target. As a demonstration, potent binders with low-to-subnanomolar K values were identified for human factor XIIa (hFXIIa) and interferon-gamma receptor 1, from a library of their 10 members. One of the anti-hFXIIa macrocyclic peptides that exhibited a high inhibitory activity and serum stability was co-crystallized with hFXIIa. The X-ray structure revealed that it adopts an antiparallel β-sheet structure induced by a (1S,2S)-2-ACHC residue via the formation of two γ-turns. This work demonstrates the potential of this platform to explore the previously inaccessible sequence space of cβAA-containing peptides.
含有β-氨基酸的肽显示出稳定的二级结构,如螺旋和片层,通常被称为折叠体。由于其受限的构象,环状β-氨基酸(cβAAs),如 2-氨基环己烷羧酸(2-ACHC),是很强的螺旋/转角诱导剂。在这里,我们通过遗传密码重编程报告了含有多个(多达 10 个)连续 cβAA 的折叠体肽的核糖体合成。我们还报告了能够结合蛋白质靶标的新的环状 cβAA 肽的从头发现。作为一个演示,从它们的 10 个成员的文库中,鉴定出了针对人凝血因子 XIIa(hFXIIa)和干扰素-γ受体 1 的具有低至亚纳摩尔 K 值的强结合物。与 hFXIIa 共结晶的一种具有高抑制活性和血清稳定性的抗 hFXIIa 环肽,其 X 射线结构表明它通过形成两个γ-转角,采用由(1S,2S)-2-ACHC 残基诱导的反平行 β-折叠结构。这项工作证明了该平台探索以前无法进入的 cβAA 肽序列空间的潜力。
