2023
DOI: 10.3390/pharmaceutics15061698
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Potent and Selective Benzothiazole-Based Antimitotics with Improved Water Solubility: Design, Synthesis, and Evaluation as Novel Anticancer Agents

Abstract: The design of colchicine site ligands on tubulin has proven to be a successful strategy to develop potent antiproliferative drugs against cancer cells. However, the structural requirements of the binding site endow the ligands with low aqueous solubility. In this work, the benzothiazole scaffold is used to design, synthesize, and evaluate a new family of colchicine site ligands exhibiting high water solubility. The compounds exerted antiproliferative activity against several human cancer cell lines, due to tub… Show more

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Cited by 7 publications
(8 citation statements)
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“…These results suggest that the replacement of the phenyl ring by the smaller ethyl groups requires a compensating increase in volume on the BZT moiety, and the observed differences might result from different binding modes. As anticipated, most of the synthesized compounds did not show antiproliferative activity, thus reflecting the strict structural requirements for eliciting antiproliferative activity, which is in good agreement with many previous studies on colchicine-site ligands showing that structural variations resulted in large potency changes [22,24,28,50]. Frentizole, although not the most potent antiproliferative agent of the series, has the broader antiproliferative profile and is, therefore, the optimal candidate for repurposing.…”
Section: Discussionsupporting
confidence: 88%
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“…These results suggest that the replacement of the phenyl ring by the smaller ethyl groups requires a compensating increase in volume on the BZT moiety, and the observed differences might result from different binding modes. As anticipated, most of the synthesized compounds did not show antiproliferative activity, thus reflecting the strict structural requirements for eliciting antiproliferative activity, which is in good agreement with many previous studies on colchicine-site ligands showing that structural variations resulted in large potency changes [22,24,28,50]. Frentizole, although not the most potent antiproliferative agent of the series, has the broader antiproliferative profile and is, therefore, the optimal candidate for repurposing.…”
Section: Discussionsupporting
confidence: 88%
“…Accordingly, the docking results place the cis isomer within the AB subpockets and the trans isomer within the AC ones. In the first instance, the BZT ring is located in the B zone and the phenyl ring in the region between the A the C zones, as previously described by us for related ureas [50]. For the trans isomer, the BZT is allocated to the A zone, similar to MI-181 [36], and the phenyl ring toward the C zone.…”
Section: Docking Studiesmentioning
confidence: 76%
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