Study of the Binding Site of Long Chain Fatty Acids on Fatty Acid-Binding Proteins

Z. Tarhda
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Abstract

Fatty acid binding proteins (FABPs) are proposed to function in the transport, metabolism, or storage of free fatty acids. Despite extensive studies, the mechanism of fatty acid binding and the ability of FABPs to discriminate among fatty acids according to their chain lengths and saturation state are poorly understood. In this work, we aimed to study the key features of FABP binding site based on the crystallographic structure of FABP-LCFA complexes, sequence multiple alignment and structural superposition of some FABPs. Due to the important role of the physicochemical features of the proteins in the ligand interaction, we studied those of the FABPs. The nature of the bond between the FABPs and the different LCFA, also the part of LCFA involved in LCFA-FABP interaction is interesting to detect the mechanism of LCFAs binding on FABPs. To achieve these objectives, we used different databases and various bioinformatics programs. Based on the results, we were able to answered some unclear about the mechanism of fatty acid binding.
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长链脂肪酸与脂肪酸结合蛋白结合位点的研究
脂肪酸结合蛋白(FABPs)被认为在游离脂肪酸的运输、代谢或储存中起作用。尽管进行了广泛的研究,但脂肪酸结合的机制以及FABPs根据其链长和饱和状态区分脂肪酸的能力尚不清楚。在这项工作中,我们旨在基于FABP- lcfa配合物的晶体结构,序列多重比对和一些FABP的结构叠加来研究FABP结合位点的关键特征。由于蛋白质的物理化学特征在配体相互作用中的重要作用,我们研究了FABPs的物理化学特征。研究FABPs与不同LCFA之间的结合性质,以及LCFA参与LCFA- fabp相互作用的部分,对检测LCFA与FABPs结合的机制很有意义。为了实现这些目标,我们使用了不同的数据库和各种生物信息学程序。在此基础上,我们能够回答一些不清楚的脂肪酸结合机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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