Benzothiazole derivatives as human DNA topoisomerase IIα inhibitors

Özen, Çigdem; Tekiner-Gülbaş, Betül; Foto, Egemen; Yildiz, İ̇lkay; Dırıl, Nuran; Aki, Esin; Yalçın, İsmail

doi:10.1007/s00044-013-0577-5

Cited by 18 publications

(16 citation statements)

References 31 publications

(25 reference statements)

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“…In this study, we used fast flexible docking to study the binding orientations and predict binding affinities of benzothiazole and benzothiazolium derivatives. Such studies have been carried out to understand the forms of interaction of 12 compounds, examined by Kaplan-Ozen and colleagues for human DNA topoisomerases [21]. The results obtained from this study will be useful in understanding the inhibitory mode of benzothiazole and benzothiazolium derivatives, as well as in rapidly and accurately predicting the activities of newly designed inhibitors on the basis of docking scores.…”

Section: Introductionmentioning

confidence: 99%

“…A set of previously synthesized benzothiazole and 3-amino-benzothiazolium derivatives [16] tested for DNA topoisomerase II inhibitory activity were chosen from our previous study [21] as shown in Table 1. The DNA topoisomerase II inhibitory activities of these compounds are represented as IC 50 values in the millimolar, micromolar or nanomolar range [21].…”

Section: Molecular Structures and Optimizationmentioning

confidence: 99%

“…Our group has been working for many years on the synthesis of some new heterocyclic compounds that were potentially DNA topoisomerase I and II inhibitors, and molecular modelling studies of these compounds [15][16][17][18][19][20][21]. So far some of the compounds exhibited significant topoisomerase II inhibitory activity with IC 50 values differing from 11.4 and 46.8 μM compared with the standard drug etoposide [15,18].…”

Section: Introductionmentioning

confidence: 99%

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Evaluation of inhibitory effects of benzothiazole and 3-amino-benzothiazolium derivatives on DNA topoisomerase II by molecular modeling studies

Akı-Yalçın

Ertan-Bolelli

Tok

et al. 2014

SAR and QSAR in Environmental Research

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There has been considerable interest in DNA topoisomerases over the last decade, as they have been shown to be one of the major cellular targets in anticancer drug development. Previously we synthesized some benzothiazole derivatives and corresponding benzothiazolium forms, and tested their DNA inhibitory activity to develop novel antitumor agents. Among the 12 prepared compounds, compound BM3 (3-aminobenzothiazole-3-ium 4-methylbenzene sulfonate) exhibited extreme topoisomerase II inhibitory activity compared with the reference drug etoposide. We also tried to determine the DNA and enzyme binding abilities of BM3 and found that BM3 acted on topoisomerase II first at low doses, while it had also showed DNA minor groove binding properties at higher doses. In this study the interactions between DNA topoisomerase II and the compounds were examined in detail by molecular modelling studies such as molecular docking and pharmacophore analysis performed using Discovery Studio 3.5. As a result, it was found that benzothiazolium compounds exhibited a totally different mechanism than benzothiazoles by binding to the different amino acids at the active site of the protein molecule. 3-Aminobenzothiazoliums are worthy of carrying onto anticancer studies; BM3 especially would be a good anticancer candidate for preclinical studies.

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Section: Introductionmentioning

confidence: 99%

Section: Molecular Structures and Optimizationmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Evaluation of inhibitory effects of benzothiazole and 3-amino-benzothiazolium derivatives on DNA topoisomerase II by molecular modeling studies

Akı-Yalçın

Ertan-Bolelli

Tok

et al. 2014

SAR and QSAR in Environmental Research

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“…Some of the benzoxazole and benzamide compounds, which were previously synthesized in our laboratory, showed strong inhibitory activity for human DNA Topoisomerases and Glutathione S-Transferases and also anticancer effects observed on various cell cultures [12][13][14][15][16][17][18][19][20]. These findings encouraged us to search for the new anticancer target NK1R by comparing their activities with the well-known NK1R antagonist aprepitant.…”

Section: Introductionmentioning

confidence: 99%

“…Over the last decade our group have been working on the drug design studies on the new anticancer active compounds by using both computational techniques and experimental work such as synthesis and activity studies [12][13][14][15][16][17][18][19][20]. Some of the benzoxazole and benzamide compounds, which were previously synthesized in our laboratory, showed strong inhibitory activity for human DNA Topoisomerases and Glutathione S-Transferases and also anticancer effects observed on various cell cultures [12][13][14][15][16][17][18][19][20].…”

Section: Introductionmentioning

confidence: 99%

Possible Mechanism of Action of Neurokinin-1 Receptors (NK1R) Antagonists

Ozturk¹,

Akı-Yalçın²,

Ertan-Bolelli³

et al. 2017

JPP

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Abstract:Recently, NK1R (Neurokinin-1 receptors) take attention as new and promising target in anticancer drug development area. It has been proved that non-peptide NK1R antagonists L-733,060, aprepitant and L-732,138 inhibited tumor growth in several cancer cell lines. For the development of novel NK1R antagonists as antitumor agents, heterocyclic compounds which were previously synthesized by our team, tested for their cytotoxic activities in several cancer cell lines in this study. Among the tested compounds, a benzothiazole derivative BSN-009 inhibited colon cancer cell lines growth by 57.53% by comparing the activity to the control drug aprepitant. Molecular modeling studies such as molecular docking and pharmacophore generation were performed with known NK1R antagonists and BSN-009 by using Discovery Studio 3.5 in order to explain their binding modes to NK1R. BSN-009 may be a good anticancer drug candidate as a possible NK1R antagonist and is worthy to carry on the anticancer studies.

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Design, Synthesis, and Anticancer Activity of Novel Benzothiazole Analogues

Hassan

Sarg

Hussein

2019

Journal of Heterocyclic Chem

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On the pharmaceutical account of the reported anticancer activity of benzothiazole derivatives, differently substituted benzothiazole derivatives 2a–c to 34a,b, attached at 2‐position to different heterocyclic moieties, were synthesized via different chemical reactions. Thirteen of the newly synthesized compounds were selected by the National Cancer Institute, Bethesda, Maryland, USA, and evaluated for their in vitro antitumor activity against 60 human tumor cell lines in a one‐dose screening panel among which two compounds 4 and 17 showed high activity and were selected for further evaluation in the five‐dose full panel assay, in which compound 4 exerted powerful growth inhibitory activity against all cell lines with GI50 ranging from 0.683 to 4.66 μM/L in addition to excellent lethal activity against most of the cell lines.

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Benzothiazole derivatives as human DNA topoisomerase IIα inhibitors

Cited by 18 publications

References 31 publications

Evaluation of inhibitory effects of benzothiazole and 3-amino-benzothiazolium derivatives on DNA topoisomerase II by molecular modeling studies

Evaluation of inhibitory effects of benzothiazole and 3-amino-benzothiazolium derivatives on DNA topoisomerase II by molecular modeling studies

Possible Mechanism of Action of Neurokinin-1 Receptors (NK1R) Antagonists

Design, Synthesis, and Anticancer Activity of Novel Benzothiazole Analogues

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