视黄醇结合蛋白-3和视网膜s抗原在Eales病中的比较建模及使用计算方法预测其结合位点。

Anshul Tiwari, Ashish Chandra Trivedi, Prachi Srivastava, Aditya Bhusan Pant, Sandeep Saxena
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引用次数: 8

摘要

视网膜s抗原和光感受器间类视黄酸结合蛋白-3在Eales病的发病过程中起重要作用。蛋白质三维结构在功能上非常重要,在疾病的进展中起着重要的作用,因此这些三维结构是进一步药物设计和相关研究的更好靶点。我们建立了Eales病患者视黄醇结合蛋白-3和视网膜s抗原蛋白的三维模型结构。功能位点预测是一个非常重要和相关的步骤;因此,在目前的分析过程中,我们预测了目标蛋白中假定的功能位点残基。本研究所记录的这些Eales病蛋白的分子模型可能为设计针对Eales病的抑制剂或更好的配体提供有价值的帮助,并可能在药物设计中发挥重要作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Comparative modeling of retinol-binding protein-3 and retinal S-antigen in Eales' disease and prediction of their binding sites using computational methods.

Comparative modeling of retinol-binding protein-3 and retinal S-antigen in Eales' disease and prediction of their binding sites using computational methods.

Comparative modeling of retinol-binding protein-3 and retinal S-antigen in Eales' disease and prediction of their binding sites using computational methods.

Comparative modeling of retinol-binding protein-3 and retinal S-antigen in Eales' disease and prediction of their binding sites using computational methods.

Retinal S-antigen and interphotoreceptor retinoid-binding protein-3 play a significant role in the etiopathogenesis of Eales' disease. Protein 3D structures are functionally very important and play a significant role in progression of the disease, hence these 3D structures are better target for further drug designing and relative studies. We developed 3D model structure of retinol-binding protein-3 and retinal S-antigen protein of human involved in Eales' disease. Functional site prediction is a very important and related step; hence, in the current course of analysis, we predicted putative functional site residues in the target proteins. Molecular models of these proteins of Eales' disease as documented in this study may provide a valuable aid for designing an inhibitor or better ligand against Eales' disease and could play a significant role in drug design.

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