2023
DOI: 10.1080/14756366.2023.2242714
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Design and synthesis of new spirooxindole candidates and their selenium nanoparticles as potential dual Topo I/II inhibitors, DNA intercalators, and apoptotic inducers

Samar El-Kalyoubi,
Mohamed M. Khalifa,
Mahmoud T. Abo-Elfadl
et al.

Abstract: A new wave of dual Topo I/II inhibitors was designed and synthesised via the hybridisation of spirooxindoles and pyrimidines. In situ selenium nanoparticles (SeNPs) for some derivatives were synthesised. The targets and the SeNP derivatives were examined for their cytotoxicity towards five cancer cell lines. The inhibitory potencies of the best members against Topo I and Topo II were also assayed besides their DNA intercalation abilities. Compound 7d NPs exhibited … Show more

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Cited by 15 publications
(5 citation statements)
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“…Dox is generally used as a positive control and widespread chemotherapeutic drug owing to its multiple modes of action (e.g., topoisomerase II inhibition and intercalation into DNA). 55,56 Intriguingly, among the investigated OSe compounds, 8 manifested the best mean GI% (64.60%) in comparison to Dox which displayed a GI% of 70.22%. Moreover, low GI% values were attained by the investigated OSe compounds against the utilized normal cell lines assuring their safety and selectivity to cancer cells.…”
Section: Biological Evaluationmentioning
confidence: 92%
“…Dox is generally used as a positive control and widespread chemotherapeutic drug owing to its multiple modes of action (e.g., topoisomerase II inhibition and intercalation into DNA). 55,56 Intriguingly, among the investigated OSe compounds, 8 manifested the best mean GI% (64.60%) in comparison to Dox which displayed a GI% of 70.22%. Moreover, low GI% values were attained by the investigated OSe compounds against the utilized normal cell lines assuring their safety and selectivity to cancer cells.…”
Section: Biological Evaluationmentioning
confidence: 92%
“…The PARP-1 inhibitory potential of the novel 4-chloropyridazinoxyphenyl hybrids ( 3a–h , 4a–e , and 5 ) was investigated using the drug design docking approach. 56,57 All members were transferred from ChemDraw to the working window to be prepared through partial charge optimization and energy minimization steps. 58 The Protein Data Bank website was used to download the target PARP-1 receptor (PDB ID: ) which was prepared by correcting the missed parts, adding the 3D hydrogens, and minimizing its energy.…”
Section: Methodsmentioning
confidence: 99%
“…All compounds were ranked according to their affinities towards the target receptors and the best ones were selected for further investigation. On the other side, validation processes were carried out for the cocrystal inhibitors within their binding pockets, and acceptable values were obtained (RMSD < 2) (Al-Karmalawy et al, 2023;El-Kalyoubi et al, 2023).…”
Section: Molecular Docking Studies and Heat Map Analysismentioning
confidence: 99%