In Silico Profiling of Histone Deacetylase 8 Inhibitory Activity: A Computational Analysis of Novel Dipeptide-Based Compounds Cross-Linked with Hydroxamic Acid

Omer mohammed Ammash, S. Alwan, A. R. Albakaa, İsmail Alshrif, Ibrheam ben Sulaiman
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Abstract

This study involved the development of innovative compounds consisting of dipeptide cross-links combined with hydroxamic acid. Our objective was to assess their binding affinities with histone deacetylase 8 (HDAC8) by conducting a docking study, comparing the results with the reference ligand, suberoylanilide hydroxamic acid (SAHA). Docking scores were measured in terms of ΔG (Kcal/mol), and the recorded scores for compounds 2A-D were found to be higher than that of SAHA, with values of 87.36, 80.46, 79.42, and 74.14, respectively. Notably, compound 2A, a dipeptide consisting of L-tryptophyl-L-tyrosine linked to a hydroxamic acid moiety, exhibited the highest docking score of 87.36. This finding suggests that compound 2A may possess the most potent HDAC8 inhibitory activity among the other designed compounds. Furthermore, we utilized the SwissADME server to predict the physicochemical properties and additional ADME parameters for the designed compounds. The analysis revealed that all investigated compounds exhibited a high potential for passive oral absorption and demonstrated no penetration into the blood-brain barrier. Compound 2A, 2B, and 2D exhibited one Lipinski's rule violation each, whereas Compound 2C demonstrated no such violations in all parameters. Additionally, compounds 2A and 2C exhibited potential as P-glycoprotein (P-gp) substrates. SAHA did not exhibit inhibition of any of the cytochrome P450 (CYP) enzymes used in this study, whereas compounds 2B, 2C and 2D displayed possible inhibitory activities. These compelling findings provide encouraging prospects for the future synthesis of the designed compounds and warrant further evaluation through in vitro and in vivo biological studies.  
组蛋白去乙酰化酶 8 抑制活性的硅学分析:与羟肟酸交联的新型二肽化合物的计算分析
这项研究涉及开发由二肽交联和羟肟酸组成的创新化合物。我们的目的是通过进行对接研究,评估它们与组蛋白去乙酰化酶8(HDAC8)的结合亲和力,并将结果与参考配体亚伯酰酰苯胺羟肟酸(SAHA)进行比较。对接得分以ΔG(Kcal/mol)为单位进行测量,发现化合物2A-D的记录得分高于SAHA,分别为87.36、80.46、79.42和74.14。值得注意的是,化合物 2A 是由 L-色氨酰-L-酪氨酸与羟肟酸连接而成的二肽,其对接得分最高,达到 87.36 分。这一发现表明,化合物 2A 可能是其他设计化合物中具有最强 HDAC8 抑制活性的化合物。此外,我们还利用 SwissADME 服务器预测了所设计化合物的理化性质和其他 ADME 参数。分析结果表明,所有研究化合物都具有较高的被动口服吸收潜力,并且没有显示出对血脑屏障的渗透作用。化合物 2A、2B 和 2D 各违反了一项利宾斯基规则,而化合物 2C 在所有参数中均未违反该规则。此外,化合物 2A 和 2C 具有作为 P 糖蛋白 (P-gp) 底物的潜力。SAHA 对本研究中使用的任何细胞色素 P450 (CYP) 酶都没有抑制作用,而化合物 2B、2C 和 2D 则显示出可能的抑制活性。这些令人信服的发现为今后合成所设计的化合物提供了令人鼓舞的前景,值得通过体外和体内生物学研究进行进一步评估。
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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