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Molecular docking analysis of nitisinone with homogentisate 12 dioxygenase

机译:尼古丁酮与高纯尿酸12双加氧酶的分子对接分析

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摘要

Alkaptonuria is an inherited disease that is caused by homogenticate accumulation. Deficiency or mutation in Homogentisate 1,2 dioxygenase gene (chromosome 3q21-q23) leads to production of incorrectly folded or truncated enzyme. Several studies indicated that competitive inhibitors of Homogentisate 1,2 dioxygenase like Nitisinone could be used for Alkaptonuria treatment. Therefore, it is of interest to design better inhibitors of the enzyme. We used subset 3_p.0.5 from Zinc database as the virtual screening library by PyRx software relaying on Lamarckian genetics algorithm. Top 10 hits with more efficient binding affinity were analyzed and hit No#5 and No# 7 was selected for further design. In Lig No#5, we decreased the hydrophobicity by adding oxygen in the hydrophobic tail of the molecule at positions C5 and C10. The new compound of (2Z, 5Z, 8Z)-6,9-Dihydroxy-2-(2-hydroxy-5-oxo-1,3-cyclohexadien-1-yl)-2,5,8-decatrienoic acid satisfied Lipinski rules as well as PhysChem and FafDrugs filters. Moreover, the modified version of Lig No# 7 with the IUPAC name of [2-(Carboxymethyl)-3,5-dihydroxyphenyl] acetic acid satisfies the Lipisnki, FafDrugs and Physchem.
机译:碱性酮尿症是由匀浆积累引起的遗传性疾病。纯合子1,2双加氧酶基因(染色体3q21-q23)的缺乏或突变会导致产生错误折叠或截断的酶。几项研究表明,同种药1,2,Noxygenase的竞争性抑制剂(如尼替尼酮)可用于碱性磷酸酶尿症的治疗。因此,感兴趣的是设计更好的酶抑制剂。我们使用了基于Lamarckian遗传算法的PyRx软件,将Zinc数据库中的3_p.0.5子集用作虚拟筛选库。分析了具有更有效结合亲和力的前10个命中,并选择了No#5和No#7进行进一步设计。在5号接头中,我们通过在分子C5和C10的疏水尾中添加氧来降低疏水性。 (2Z,5Z,8Z)-6,9-二羟基-2-(2-羟基-5-氧代-1,3-环己二-1-基)-2,5,8-十二碳烯酸的新化合物满足Lipinski规则以及PhysChem和FafDrugs过滤器。此外,具有IUPAC名称为[2-(羧甲基)-3,5-二羟基苯基]乙酸的Lig No#7的改性形式满足Lipisnki,FafDrugs和Physchem。

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