对 Oroxylum indicum vent 化合物在治疗和预防鼻咽癌方面的合理性进行硅学评估。

IF 1.7 Q3 INTEGRATIVE & COMPLEMENTARY MEDICINE
Saketh Ram Thrigulla , Gagandeep Singh , Hemant Soni , Smriti Tandon , Shruti Koulgi , Mallikarjunachari V.N. Uppuladinne , Vinod Jani , Uddhavesh Sonavane , Rajendra Joshi , Yashika Gandhi , Vijay Kumar , Vaibhav Charde , Sujeet K. Mishra , Mukesh Chincholikar , Rakesh Narayan , Vinod Lavaniya , Ch Venkata Narasimhaji , Narayanam Srikanth , Rabinarayan Acharya
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引用次数: 0

摘要

背景:Shyonaka(Oroxylum indicum Vent)在阿育吠陀和民族医学中被广泛用于治疗炎症、疼痛、腹泻、不愈合溃疡和癌症。由于鼻咽癌(NPC)患者中爱泼斯坦-巴尔病毒(EBV)感染率较高,同时靶向参与 EBV 复制和鼻咽癌增殖的蛋白质可能有助于有效控制疾病:本研究旨在从 Oroxylum indicum 中发现潜在的双靶向抑制剂,这些抑制剂具有同时抑制 EBV 和鼻咽癌的潜力。本研究还尝试对Syonaka树皮煎剂(SBD)进行定量分析,以确认Syonaka的主要标记化合物黄芩苷(Baicalein)和菊苷(Chrysin)的存在:对 Oroxylum indicum 的茎皮和根皮进行高效液相色谱分析,以估计标记化合物 Baicalein 和 Chrysalin 的存在。硅内分析包括 ADMET 分析,然后使用 DOCK6 工具将从 Oroxylum indicum 中提取的已知化合物(从 IMPPAT 数据库中检索)与 EBV(BHRF1、NEC1、dUTPase、Uracil DNA 糖基化酶)和 NPC(COX-2、EGFR 和 MDM2)的靶蛋白进行分子对接。使用 AMBER20 软件包对筛选出的顶级分子与选定靶蛋白的分子动力学模拟进行了进一步验证,并计算了其相应的 MMGBSA 结合自由能值:结果:分子对接显示,来自植物的关键分子,黄芩苷 7-芸香糖苷 (S7R)、黄芩苷 (SCU) 和 6-羟基木犀草素、黄芩素和 5,7-二羟基-2-苯基-6-[3,4、5-三羟基-6-(羟甲基)氧杂环丁烷-2-基]氧苯并吡喃-4-酮(57D)可有效干预鼻咽癌主要致病因子之一 EBV 的靶蛋白,是鼻咽癌的特异性靶点,具有缩小肿瘤体积和减轻鼻咽癌其他后果的潜力。S7R, Baicalein和57D, Baicalein分别与MDM-2蛋白和dUTP酶蛋白的分子动力学模拟显示了它们之间稳定的相互作用,并进一步通过结合能计算进行了评估:总之,这些植物化学物质与靶蛋白的体内评估表明,它们具有抑制 EBV 和鼻咽癌的潜力,这需要进一步的体外和体内验证。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
In-silico evaluation of Oroxylum indicum vent compounds in the plausible treatment and prevention of nasopharyngeal cancer

Background

Shyonaka (Oroxylum indicum Vent) is widely used in Ayurveda and in ethnomedical practice for the treatment of inflammation, pain, diarrhea, non-healing ulcers, and cancer. Owing to the high prevalence of Epstein-Barr virus (EBV) infection in Nasopharyngeal carcinoma (NPC) patients, simultaneous targeting of proteins involved in both EBV replication and NPC proliferation might help to manage the disease effectively.

Objectives

This study is designed to identify potential dual targeting inhibitors from Oroxylum indicum having the potential to inhibit both EBV and NPC. This study also attempted quantitative analysis of Shyonaka Bark Decoction (SBD) to confirm the presence of Baicalein and Chrysin which are predominant marker compounds of Shyonaka.

Methodology

The HPLC analysis of stem bark and root bark of Oroxylum indicum was done to estimate the presence of marker compounds Baicalein and Chrysalin. The in-silico analysis included ADMET analysis followed by molecular docking of known compounds from Oroxylum indicum (retrieved from IMPPAT database) onto the target proteins of EBV (BHRF1, NEC1, dUTPase, Uracil DNA glycosylase) and NPC (COX-2, EGFR, and MDM2) using DOCK6 tool. Further validations were done using the molecular dynamics simulations of top screened molecules onto the selected target proteins using AMBER20 package and their corresponding MMGBSA binding free-energy values were calculated.

Results

The molecular docking revealed that the key molecules from the plant, scutellarein 7-rutinoside (S7R), scutellarin (SCU) and 6-hydroxyluteolin, Baicalein and 5,7-Dihydroxy-2-phenyl-6-[3,4,5-trihydroxy-6-(hydroxymethyl)oxan-2-yl]oxychromen-4-one (57D) are effectively intervening with the target proteins of EBV, one of the key causative factors of NPC and the NPC specific targets which have the potential to reduce tumor size and other consequences of NPC. The molecular dynamics simulations of S7R, Baicalein and 57D, Baicalein with MDM-2 protein and dUTPase protein, respectively, showed stable interactions between them which were further assessed by the binding energy calculations.

Conclusion

Overall, the in-silico evaluation of these phytochemicals with target proteins indicates their potential to inhibit both EBV and NPC which needs further in-vitro and in-vivo validations.

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来源期刊
Journal of Ayurveda and Integrative Medicine
Journal of Ayurveda and Integrative Medicine INTEGRATIVE & COMPLEMENTARY MEDICINE-
CiteScore
4.70
自引率
12.50%
发文量
136
审稿时长
30 weeks
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