Synthesis, Molecular Docking and Anticancer Activity of Some 5‐Aryl‐5,10‐dihydropyrido[2,3‐d:6,5‐d′]dipyrimidine‐2,4,6,8‐tetraone Derivatives and Pyrido[2,3‐d]pyrimidines
Abstract:A novel and efficient route towards the synthesis of pyrido [2,3d:6,5-d']dipyrimidines 4 a-g as unexpected products through the reaction of 6-aminouracil (1) and arylidenemalononitrile or ethyl arylidenecyanoacetate in acetic acid were investigated. On the other hand, reaction of 6-aminouracil and ethyl 4nitrobenzylidenecyanoacetate in ethanol in presence of piperidine (few drops) afforded pyrido[2,3-d]pyrimidine-6-carbonitrile 5. In addition, pyrido[2,3-d]pyrimidines 6 a-g were obtained through the reaction o… Show more
“…The compounds were elucidated by using IR, 1 H-NMR, 13 C-NMR and mass spectra, in addition to revealing their actual influence on human cancer (HEPG-2) and (MCF-7), antioxidant, antimicrobial, and fluoresceine properties, but the main biological activity on this protocol was as anticancer on human cancer (HEPG-2) and (MCF-7) and supported by docking studies due to these cells are the most frequent tumors in Egypt and more authentic cells, available for the cytotoxicity of compounds. [21] Some synthetized compound in this work showed the potent activity against cancer cell lines MCF-7 and HEPG2 cell so we also screen their effecting on the normal cell. The experimental data were provided by computational studies (molecular docking and 2D-QSAR modeling) by using MOE (2015).…”
2,2' (2,4-dioxopentane-3,3-diyl) bis(diazene-2,1-diyl) dibenzoic acid was produced in this work, which was derived from the coupling reaction between two moles of diazonium salt and one mole of acetylacetone in an alkaline medium. Some derivatives based on this starting material were investigated. The structures of the good yielded synthesized composites were well characterized by different spectral techniques such as IR, 1 H-NMR, 13 C-NMR, and mass spectrometry. Due to the outrageous spread of cancer, these compounds were tested for the cytotoxicity against human tumor cells (HEPG-2) and (MCF-7) as a wide spread type of cancers in Egypt. The study illustrated that compounds 11a and 11b had a very powerful effect on two separate cell lines (HEPG-2 and MCF-7) and compounds 8 and 6 had a strong effect. The results of anticancer were supported by molecular docking and 2D-QSAR modeling. In addition to testing the compounds as anticancer drugs, they were examined as antioxidant by using [DPPH] technique, antimicrobial activity (gram-positive and gramnegative) and antifungal activity which provided satisfactory results. The fluorescence properties were tested as an analytical application for the produced substances with good results.
“…The compounds were elucidated by using IR, 1 H-NMR, 13 C-NMR and mass spectra, in addition to revealing their actual influence on human cancer (HEPG-2) and (MCF-7), antioxidant, antimicrobial, and fluoresceine properties, but the main biological activity on this protocol was as anticancer on human cancer (HEPG-2) and (MCF-7) and supported by docking studies due to these cells are the most frequent tumors in Egypt and more authentic cells, available for the cytotoxicity of compounds. [21] Some synthetized compound in this work showed the potent activity against cancer cell lines MCF-7 and HEPG2 cell so we also screen their effecting on the normal cell. The experimental data were provided by computational studies (molecular docking and 2D-QSAR modeling) by using MOE (2015).…”
2,2' (2,4-dioxopentane-3,3-diyl) bis(diazene-2,1-diyl) dibenzoic acid was produced in this work, which was derived from the coupling reaction between two moles of diazonium salt and one mole of acetylacetone in an alkaline medium. Some derivatives based on this starting material were investigated. The structures of the good yielded synthesized composites were well characterized by different spectral techniques such as IR, 1 H-NMR, 13 C-NMR, and mass spectrometry. Due to the outrageous spread of cancer, these compounds were tested for the cytotoxicity against human tumor cells (HEPG-2) and (MCF-7) as a wide spread type of cancers in Egypt. The study illustrated that compounds 11a and 11b had a very powerful effect on two separate cell lines (HEPG-2 and MCF-7) and compounds 8 and 6 had a strong effect. The results of anticancer were supported by molecular docking and 2D-QSAR modeling. In addition to testing the compounds as anticancer drugs, they were examined as antioxidant by using [DPPH] technique, antimicrobial activity (gram-positive and gramnegative) and antifungal activity which provided satisfactory results. The fluorescence properties were tested as an analytical application for the produced substances with good results.
“…Unexpectedly, Farag et al [ 82 ] efficiently prepared pyridodipyrimidines 46a – g (Scheme 23 ) in a one-step synthesis. Therefore, the reactions of 6-amino-uracil with arylidene-malononitrile or ethyl arylidene-cyanoacetate gave the desired products in respectable to exceptional yields.…”
Section: Synthetic Approachesmentioning
confidence: 99%
“…The compounds are more applicable to hinder the growth of HePG2 cells in most of the cases except in the case of compounds 46b (Ar = 4-NO 2 -C 6 H 4 ) (IC 50 = 68.59 ± 3.6 µM), 46e (Ar = 4-MeO-C 6 H 4 ) (IC 50 = 42.63 ± 2.8 µM), and 46f (IC 50 = 35.91 ± 2.5 µM), against HCT-116 cells, along with the potency of compound 46 g (Ar = 4-OH-C 6 H 4 ) (IC 50 = 49.87 ± 3.0 µM) against MCF-7 tumor cells. The comparison of the cytotoxic results against the investigated cell lines with the chemotherapeutic standards indicated that the compounds displayed moderate to weak cytotoxic activities based on the scale of comparison that referred to the moderate impacts in the range of IC 50 = 21 to 50 µM along with the weak cytotoxic influences for IC 50 values higher than 50 µM [ 82 ]. Fig.…”
Section: Biological Activities Of Pyridodipyrimidine Derivativesmentioning
The entitled review aimed to assemble and highlight the synthetic approaches and biological aspects of heterocycles with pyridodipyrimidine motifs. The recent synthetic approaches were categorized according to the accomplishments of the approaches under catalyst or catalyst-free conditions. The topic involved the synthesis of substituted tricyclic systems and spirocyclic systems. The present study offered an overview of the recent literature in addition to a scope of the preceding literature. The proposed mechanisms of the varied target products were discussed. Pyridodipyrimidine displayed potential and privileged cytotoxic, antioxidant, and antimicrobial performances. The competitions, challenges, and prospects are also deliberated.
“…Farag et al [39] synthesised novel pyrido ). The synthesised compounds were appraised for its antiproliferative activity towards human hepatocarcinoma (HEPG-2), human colon carcinoma (HCT-116) and human mammary carcinoma (MCF-7) cell lines [40] It was observed that Anti HCV Kayali et al [23] Sofosbuvir 2.…”
This review article delves into the intricate biological activities of uracil, an essential pyrimidine Base pivotal in RNA structures. Examining its involvement in nucleic acid metabolism, various multifunctional roles, spanning from influencing cell proliferation to its antimicrobial and antiviral properties. The study explores signal transduction pathways affected by uracil, unraveling potential therapeutic applications. By unraveling the nuanced biological mechanisms. This review contributes to a deeper understanding of uracil's impact, offering insights crucial for drug development and advancing biomedical research.
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