Vettorazzi Marcela, Angelina Emilio, Lima Santiago, Gonec Tomas, Otevrel Jan, Marvanova Pavlina, Padrtova Tereza, Mokry Petr, Bobal Pavel, Acosta Lina M, Palma Alirio, Cobo Justo, Bobalova Janette, Csollei Jozef, Malik Ivan, Alvarez Sergio, Spiegel Sarah, Jampilek Josef, Enriz Ricardo D
Facultad de Química, Bioquímica y Farmacia, Universidad Nacional de San Luis, Instituto Multidisciplinario de Investigaciones Biológicas (IMIBIO-SL), Chacabuco 915, 5700 San Luis, Argentina.
Laboratorio de Estructura Molecular y Propiedades, Área de Química Física, Departamento de Química, Facultad de Ciencias Exactas y Naturales y Agrimensura, Universidad Nacional del Nordeste, Avda. Libertad 5460, 3400 Corrientes, Argentina.
Eur J Med Chem. 2017 Oct 20;139:461-481. doi: 10.1016/j.ejmech.2017.08.017. Epub 2017 Aug 10.
Sphingosine kinase 1 (SphK1), the enzyme that produces the bioactive sphingolipid metabolite, sphingosine-1-phosphate, is a promising new molecular target for therapeutic intervention in cancer and inflammatory diseases. In view of its importance, the main objective of this work was to find new and more potent inhibitors for this enzyme possessing different structural scaffolds than those of the known inhibitors. Our theoretical and experimental study has allowed us to identify two new structural scaffolds (three new compounds), which could be used as starting structures for the design and then the development of new inhibitors of SphK1. Our study was carried out in different steps: virtual screening, synthesis, bioassays and molecular modelling. From our results, we propose a new dihydrobenzo[b]pyrimido[5,4-f]azepine and two alkyl{3-/4-[1-hydroxy-2-(4-arylpiperazin-1-yl)ethyl]phenyl}carbamates as initial structures for the development of new inhibitors. In addition, our molecular modelling study using QTAIM calculations, allowed us to describe in detail the molecular interactions that stabilize the different Ligand-Receptor complexes. Such analyses indicate that the cationic head of the different compounds must be refined in order to obtain an increase in the binding affinity of these ligands.
鞘氨醇激酶1(SphK1)是一种可产生生物活性鞘脂代谢产物——1-磷酸鞘氨醇的酶,它是癌症和炎症性疾病治疗干预中一个很有前景的新分子靶点。鉴于其重要性,这项工作的主要目标是寻找比已知抑制剂具有不同结构骨架的该酶的新型更有效抑制剂。我们的理论和实验研究使我们能够鉴定出两种新的结构骨架(三种新化合物),它们可作为设计并随后开发SphK1新抑制剂的起始结构。我们的研究分不同步骤进行:虚拟筛选、合成、生物测定和分子建模。根据我们的结果,我们提出一种新的二氢苯并[b]嘧啶并[5,4-f]氮杂䓬和两种烷基{3-/4-[1-羟基-2-(4-芳基哌嗪-1-基)乙基]苯基}氨基甲酸酯作为开发新抑制剂的初始结构。此外,我们使用QTAIM计算的分子建模研究使我们能够详细描述稳定不同配体-受体复合物的分子相互作用。此类分析表明,必须对不同化合物的阳离子头部进行优化,以提高这些配体的结合亲和力。
