三联苯
对接(动物)
小分子
单克隆抗体
化学
配体(生物化学)
分子
免疫系统
立体化学
组合化学
蛋白质-蛋白质相互作用
抗体
生物化学
生物
受体
免疫学
有机化学
医学
护理部
作者
Joanna Klimek,Oskar Kruc,Joanna Ceklarz,B.Z. Kaminska,Bogdan Musielak,Robin van der Straat,Alexander Dömlingꝉ,Tad A. Holak,Damian Muszak,Justyna Kalinowska‐Tłuścik,Łukasz Skalniak,Ewa Surmiak
出处
期刊:Molecules
[MDPI AG]
日期:2024-06-04
卷期号:29 (11): 2646-2646
被引量:1
标识
DOI:10.3390/molecules29112646
摘要
The PD-1/PD-L1 complex is an immune checkpoint responsible for regulating the natural immune response, but also allows tumors to escape immune surveillance. Inhibition of the PD-1/PD-L1 axis positively contributes to the efficacy of cancer treatment. The only available therapeutics targeting PD-1/PD-L1 are monoclonal antibody-based drugs, which have several limitations. Therefore, small molecule compounds are emerging as an attractive alternative that can potentially overcome the drawbacks of mAb-based therapy. In this article, we present a novel class of small molecule compounds based on the terphenyl scaffold that bind to PD-L1. The general architecture of the presented structures is characterized by axial symmetry and consists of three elements: an m-terphenyl core, an additional aromatic ring, and a solubilizing agent. Using molecular docking, we designed a series of final compounds, which were subsequently synthesized and tested in HTRF assay and NMR binding assay to evaluate their activity. In addition, we performed an in-depth analysis of the mutual arrangement of the phenyl rings of the terphenyl core within the binding pocket of PD-L1 and found several correlations between the plane angle values and the affinity of the compounds towards the protein.
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