Dilipkumar S, Karthik V, Gowramma B, Magesh M, Kaviarasan L
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Various spectral studies distinguished the synthetic\ndesigns of the produced compounds. The naphthoquinone derivatives were exposed to the primary\nmolecular descriptor by Molinspiration programming, and all the descriptor values are within\nthe specified value.\n\n\n\nEach of the five naphthoquinone derivatives was docked against the\nTopoisomerase II utilizing Auto Dock program 4.2.5. (PDB: 3L4K). The docking tells us that the\nstudied compounds possess significant to moderate inhibition toward the targeted enzymes.\nAmong the studied compounds, compound L3 showed the most elevated binding score (-10.66\nkcal/mol with one H-bond) than the adriamycin (-9.58 kcal/mol with two H-bonds) and compound\nL2 (- 9.86 kcal/mol with two H-bonds). The derivatives were tried for in-vitro cytotoxicity\nstudies against MCF - 7 by the SRB method. Among them, compounds L2 (28.42±3.1 μg/mL)\nand L3 (29.38±3.2 μg/mL) were the most significant ones when contrasted with the control Adriamycin\n(15.28±3.4 μg/mL).\n\n\n\nThe current research indicates that the tested compounds show anticancer action\nagainst the MCF-7 breast cancer cell line. 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引用次数: 0
摘要
目前,许多醌类衍生物已被用于抗癌药物,尤其是 1,4-萘醌类衍生物具有很强的生命力,在药物和农用化学品行业中被广泛应用于未精制物质。各种光谱研究区分了所制化合物的合成设计。通过 Molinspiration 程序对萘醌衍生物进行了主分子描述符分析,所有描述符值均在规定值范围内。各种光谱研究区分了所生成化合物的合成设计。利用 Molinspiration 程序对萘醌衍生物进行了主分子描述,所有描述值均在指定值范围内。(PDB:3L4K)与拓扑异构酶 II 进行对接。在所研究的化合物中,化合物 L3 的结合得分最高(-10.66kcal/mol,一个 H 键),高于阿霉素(-9.58 kcal/mol,两个 H 键)和化合物 L2(-9.86 kcal/mol,两个 H 键)。采用 SRB 法对这些衍生物进行了针对 MCF - 7 的体外细胞毒性研究。与对照组阿霉素(15.28±3.4 μg/mL)相比,其中化合物 L2(28.42±3.1 μg/mL)和 L3(29.38±3.2 μg/mL)的细胞毒性最为显著。本研究表明,测试化合物对 MCF-7 乳腺癌细胞株具有抗癌作用。
Synthesis, Characterization, Docking Studies, and In-vitro Cytotoxic
Activity of Some Novel 2, 3 Disubstituted Naphthalene 1,4 Dione
Derivatives
Many quinone derivatives as of now utilized for anticancer medications.
Especially, 1,4-naphthoquinones are dynamic derivatives, and it was broadly utilized in unrefined
substances in the drugs and agrochemicals industry.
In this work, we planned and combined five different moieties into 2, 3
disubstituted naphthalene-1,4-dione molecules. Various spectral studies distinguished the synthetic
designs of the produced compounds. The naphthoquinone derivatives were exposed to the primary
molecular descriptor by Molinspiration programming, and all the descriptor values are within
the specified value.
In this work, we planned and combined five different moieties into 2, 3
disubstituted naphthalene-1,4-dione molecules. Various spectral studies distinguished the synthetic
designs of the produced compounds. The naphthoquinone derivatives were exposed to the primary
molecular descriptor by Molinspiration programming, and all the descriptor values are within
the specified value.
Each of the five naphthoquinone derivatives was docked against the
Topoisomerase II utilizing Auto Dock program 4.2.5. (PDB: 3L4K). The docking tells us that the
studied compounds possess significant to moderate inhibition toward the targeted enzymes.
Among the studied compounds, compound L3 showed the most elevated binding score (-10.66
kcal/mol with one H-bond) than the adriamycin (-9.58 kcal/mol with two H-bonds) and compound
L2 (- 9.86 kcal/mol with two H-bonds). The derivatives were tried for in-vitro cytotoxicity
studies against MCF - 7 by the SRB method. Among them, compounds L2 (28.42±3.1 μg/mL)
and L3 (29.38±3.2 μg/mL) were the most significant ones when contrasted with the control Adriamycin
(15.28±3.4 μg/mL).
The current research indicates that the tested compounds show anticancer action
against the MCF-7 breast cancer cell line. Thus, the study is an attempt to advance toward the
identification of innovative anticancer drugs.
Current Bioactive CompoundsPharmacology, Toxicology and Pharmaceutics-Pharmacology, Toxicology and Pharmaceutics (all)
CiteScore
1.90
自引率
0.00%
发文量
112
期刊介绍:
The journal aims to provide comprehensive review articles on new bioactive compounds with proven activities in various biological screenings and pharmacological models with a special emphasis on stereoeselective synthesis. The aim is to provide a valuable information source of bioactive compounds synthesized or isolated, which can be used for further development of pharmaceuticals by industry and academia. The journal should prove to be essential reading for pharmacologists, natural product chemists and medicinal chemists who wish to be kept informed and up-to-date with the most important developments on new bioactive compounds of natural or synthetic origin, including their stereoeselective synthesis.
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