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Homology Modeling of Leishmanolysin (gp63) from Leishmania panamensis and Molecular Docking of Flavonoids

机译:Leishmanolysin(GP63)的同源造型来自Leishmania panmenensis和黄酮类化合物的分子对接

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摘要

Leishmaniasis is a chronic disease caused by protozoa of the distinct Leishmania genus transmitted by sandflies of the genus Phlebotomus (old world) and Lutzomyia (new world). Among the molecular factors that contribute to the virulence and pathogenesis of Leishmania are metalloproteases, e.g., glycoprotein 63 (gp63), also known as leishmanolysin or major surface protease (MSP). This protease is a zinc-dependent metalloprotease that is found on the surface of the parasite, abundant in Leishmania promastigote and amastigote. This study describes the prediction of three-dimensional (3D) structures of leishmanolysin (UniProt ID A0A088RJX7) of Leishmania panamensis employing a homology modeling approach. The 3D structure prediction was performed using the SWISS-MODEL web server. The tools PROCHECK, Molprobyty, and Verify3D were used to check the quality of the model, indicating that they are reliable. Best docking configurations were identified applying AutoDock Vina in PyRx 0.8 to obtain a potential antileishmanial activity. Biflavonoids such as lanaroflavone, podocarpusflavone A, amentoflavone, and podocarpusflavone B showed good scores among these molecules. Lanaroflavone appears to be the most suitable compound from binding affinity calculations.
机译:Leishmaniaisis是由由属杂种(古老世界)和 leutzomyia(新世界)的杂种的不同 Leishmania属的原生动物引起的慢性病。在促进毒力和发病机制的分子因素中,莱山西亚是金属蛋白酶,例如糖蛋白63(GP63),也称为Leishmanolysin或主要表面蛋白酶(MSP)。该蛋白酶是一种锌依赖性金属蛋白酶,其在寄生虫的表面上发现,在 Leishmania Promastigote和Amastigote中。本研究描述了利用同源性建模方法的LeishManolysin(Uniprot ID A0a088RJX7)的三维(三维)结构的预测。使用瑞士模型Web服务器执行3D结构预测。工具Procheck,MolProbyty和Verify3D用于检查模型的质量,表明它们是可靠的。在Pyrx 0.8中识别了最佳的对接配置,以获得潜在的抗恋盲目行程。含Lanaroflavone,Podocarpusflavone A,Amentoflavone和Podocarpusflavone B的双链类动物表现出这些分子中的得分良好。 Lanaroflavone似乎是最合适的化合物,来自结合亲和计算。

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