Novel isothiacalothrixin B analogues exhibit cytotoxic activity on human colon cancer cells in vitro by inducing irreversible DNA damage

Moorthy, Nachiappan Dhatchana; Ramalingam, Bose Muthu; Iqbal, Saleem; Mohanakrishnan, Arasambattu K.; Gunasekaran, Krishnasamy; Vellaichamy, Elangovan

doi:10.1371/journal.pone.0202903

Cited by 9 publications

(4 citation statements)

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“…Treatment of cancer cells with different doses (50–150 μM) of compound 2 for 24 induced significant DNA damage in A549 cells in a dose‐dependent manner as indicated by the increased tail intensity, tail length, tail DNA, tail moment, and olive moment (Figure 12(A) and (B)). Several anti‐cancer drugs have also shown similar effects in various cancer types [33–36] …”

Section: Resultsmentioning

confidence: 99%

Non‐Covalent Interactions in the Self‐Assembly of Dihydropyridone Supramolecules and In Vitro Anti‐Cancer Assessment in Human Lung Adenocarcinoma Cell Line (A549)

et al. 2023

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The synthesis of dihydropyridone derivatives has been reported by ring rearrangement of pyrans using iodine and formic acid as a catalyst separately. Dihydropyridones were crystallized subjected for single-crystal X-ray crystallography to acquire their structural parameters. The different non-covalent interactions involved within the supramolecular systems were studied and validated using Hirshfeld surface plot analysis. NÀ H•••O interactions between the lactam group dominate. Still, other non-covalent interactions such as CÀ Hand lone pair•••π systems act as the driving force in facilitating the self-assembly of the dihydropyridone supramolecules. The synthesized compounds were analyzed by in vitro techniques using human lung adenocarcinoma (A549) to evaluate their cytotoxic activities. Ethyl 4-(4-chlorophenyl)-5cyano-2-methyl-6-oxo-1,4,5,6-tetrahydropyridine-3-carboxylate has shown the highest cytotoxicity among all the synthesized compounds. Molecular recognition properties of the dihydropyridone compounds were also studied, employing molecular docking tools to gain insight into the binding mode inside the allosteric binding pocket of the Eg5 protein through noncovalent interactions.

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Section: Resultsmentioning

confidence: 99%

Non‐Covalent Interactions in the Self‐Assembly of Dihydropyridone Supramolecules and In Vitro Anti‐Cancer Assessment in Human Lung Adenocarcinoma Cell Line (A549)

et al. 2023

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“…Clonogenic cell survival assay : Clonogenic assays were performed on HCT116 and NCI‐H460 cells according to the reported procedure . In brief, EDOT analogues at different concentrations were incubated with cells seeded at a very low density (100 cells per well of a six‐well plate), followed by washing with Dulbecco′s phosphate‐buffered saline (DPBS) and culturing the drug‐treated cells for a further 12 days in DMEM culture medium.…”

Section: Methodsmentioning

confidence: 99%

Divergent Synthesis and Evaluation of the in vitro Cytotoxicity Profiles of 3,4‐Ethylenedioxythiophenyl‐2‐propen‐1‐one Analogues

et al. 2019

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A new series of 3,4‐ethylenedioxythiophene (EDOT)‐appended propenones were prepared by condensation reaction and their in vitro cytotoxicity effects were evaluated against five human cancer cell lines. Preliminary structure–activity relationships of EDOT‐incorporated 2‐propenone derivatives were also established. The EDOT‐appended enones demonstrated significant cytotoxicity against human cancer cell lines. The most active analogue, (E)‐3‐(2,3‐dihydrothieno[3,4‐b][1,4]dioxin‐5‐yl)‐1‐(3,4,5‐trimethoxyphenyl)prop‐2‐en‐1‐one (3 p, GI50=110 nm), severely inhibited the clonogenic potential of cancer cells, and induced cell‐cycle arrest in the G2/M phase and caused an accumulation of HCT116 colon cancer cells with >4 N DNA content. Also, 3 p exhibited weak inhibition of the enzymatic activity of human topoisomerase I. Molecular docking studies indicated preferential binding of the compounds to the ATP‐binding pocket of the human checkpoint 2 kinase (Chk2) catalytic domain, thus, identifying a novel diaryl 2‐propenone chemotype for the development of potent inhibitors of Chk2.

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“…These interactions include a pi donor hydrogen bond between GLU 12 and thiophene moiety (5.88 Å), an ionic bond between GLU 8 and nitrogen atom of nitrophenol moiety (5.28 Å). [36][37][38][39][40] In addition to three alkyl interactions between methylchloro-imidazole moiety ILE 10 and LEU 134 amino acid residues (5.03, 5.04, 5.18 Å). Five pi-alkyl interactions with VALA 18, ALA 144, ILE 10, LEU 134, HIS 82 (5.80, 6.49, 4.87, 5.89, 4.85 Å) (Fig.…”

Section: Molecular Docking Studymentioning

confidence: 99%

Synthesis, anticancer evaluation of novel hybrid pyrazole-based chalcones, molecular docking, DNA fragmentation, and gene expression: in vitro studies

Yasser,

Sroor,

El-Shorbagy

et al. 2024

RSC Adv.

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Novel isothiacalothrixin B analogues exhibit cytotoxic activity on human colon cancer cells in vitro by inducing irreversible DNA damage

Cited by 9 publications

References 50 publications

Non‐Covalent Interactions in the Self‐Assembly of Dihydropyridone Supramolecules and In Vitro Anti‐Cancer Assessment in Human Lung Adenocarcinoma Cell Line (A549)

Non‐Covalent Interactions in the Self‐Assembly of Dihydropyridone Supramolecules and In Vitro Anti‐Cancer Assessment in Human Lung Adenocarcinoma Cell Line (A549)

Divergent Synthesis and Evaluation of the in vitro Cytotoxicity Profiles of 3,4‐Ethylenedioxythiophenyl‐2‐propen‐1‐one Analogues

Synthesis, anticancer evaluation of novel hybrid pyrazole-based chalcones, molecular docking, DNA fragmentation, and gene expression: in vitro studies

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