School of Chemistry, University of Leeds, Woodhouse Lane, Leeds, LS2 9JT, UK.
Astbury Centre for Structural Molecular Biology, University of Leeds, Woodhouse Lane, Leeds, LS2 9JT, UK.
Chemistry. 2020 Jun 18;26(34):7638-7646. doi: 10.1002/chem.202000417. Epub 2020 May 26.
Protein-protein interactions (PPIs) control virtually all cellular processes and have thus emerged as potential targets for development of molecular therapeutics. Peptide-based inhibitors of PPIs are attractive given that they offer recognition potency and selectivity features that are ideal for function, yet, they do not predominantly populate the bioactive conformation, frequently suffer from poor cellular uptake and are easily degraded, for example, by proteases. The constraint of peptides in a bioactive conformation has emerged as a promising strategy to mitigate against these liabilities. In this work, using peptides derived from hypoxia-inducible factor 1 (HIF-1α) together with dibromomaleimide stapling, we identify constrained peptide inhibitors of the HIF-1α/p300 interaction that are more potent than their unconstrained sequences. Contrary to expectation, the increased potency does not correlate with an increased population of an α-helical conformation in the unbound state as demonstrated by experimental circular dichroism analysis. Rather, the ability of the peptide to adopt a bioactive α-helical conformation in the p300 bound state is better supported in the constrained variant as demonstrated by molecular dynamics simulations and circular dichroism difference spectra.
蛋白质-蛋白质相互作用(PPIs)几乎控制着所有的细胞过程,因此已成为开发分子治疗药物的潜在靶点。基于肽的 PPI 抑制剂具有吸引力,因为它们具有识别效力和选择性特征,非常适合功能,但它们不会主要占据生物活性构象,经常受到细胞摄取不良的影响,并且容易被蛋白酶降解。肽在生物活性构象中的约束已成为减轻这些缺陷的有前途的策略。在这项工作中,我们使用缺氧诱导因子 1(HIF-1α)衍生的肽和二溴马来酰亚胺订书钉,确定了 HIF-1α/p300 相互作用的约束肽抑制剂,其比未约束的序列更有效。与预期相反,如实验圆二色性分析所示,增加的效力与未结合状态下 α-螺旋构象的增加群体不相关。相反,如分子动力学模拟和圆二色性差谱所示,在 p300 结合状态下,约束变体更有利于肽采用生物活性 α-螺旋构象。
