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天然酚类化合物的分子对接筛选尿素酶抑制剂。

Molecular Docking of Natural Phenolic Compounds for the Screening of Urease Inhibitors.

机构信息

International Institute of Pharmaceutical Sciences, Sonepat, Haryana, India.

Faculty of Pharmaceutical Sciences, Maharshi Dayanand University, Rohtak, Haryana, India.

出版信息

Curr Pharm Biotechnol. 2019;20(5):410-421. doi: 10.2174/1389201020666190409110948.

Abstract

BACKGROUND

Bacterial ureases have been the cause of various human and animal pathogenicity including hepatic encephalopathy, hepatic coma urolithiasis, gastric and peptic ulcers, pyelonephritis, and urinary catheter encrustation by the production of ammonia. Hence, in view of the side effects of existing drugs, there is a strong need to discover, more safe, effective and potent compounds for the treatment of infections caused by urease.

METHODS

For this purpose, several natural phenolic compounds have been screened by molecular modelling techniques, wherein the phenolic compounds were docked to the active site of Jack bean urease (PDB ID 3LA4) using the Schrodinger docking software.

RESULTS

The lead compounds were identified via in-silico screening technique where docking score, binding energy, ADME and toxicity data were considered to screen the lead compounds as compared with the available standard drugs. From the docking study of screened natural phenolic compounds, five compounds diosmin, morin, chlorogenic acid, capsaicin and resveratrol were selected based upon their better affinity towards the receptor and were considered for further wet lab studies.

CONCLUSION

The in-silico results were confirmed by in vitro experiments by use of the Jack bean urease using Weatherburn method.

摘要

背景

细菌脲酶是引起人类和动物各种致病性的原因,包括肝性脑病、肝昏迷、尿石症、胃溃疡和十二指肠溃疡、肾盂肾炎和泌尿道导管结垢,因为其产生的氨。因此,鉴于现有药物的副作用,强烈需要发现更安全、更有效和更有效的化合物来治疗由脲酶引起的感染。

方法

为此,通过分子建模技术筛选了几种天然酚类化合物,其中使用 Schrödinger 对接软件将酚类化合物对接至 Jack bean 脲酶(PDB ID 3LA4)的活性部位。

结果

通过虚拟筛选技术鉴定了先导化合物,其中对接评分、结合能、ADME 和毒性数据被用于筛选先导化合物,与现有标准药物进行比较。从筛选出的天然酚类化合物的对接研究中,根据其与受体的更好亲和力选择了 5 种化合物(柚皮苷、桑色素、绿原酸、辣椒素和白藜芦醇),并考虑进行进一步的湿实验室研究。

结论

通过使用 Weatherburn 法的 Jack bean 脲酶对体外实验的计算机结果进行了验证。

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