Synthesis of novel psoralen analogues and their in vitro antitumor activity

Francisco, Carla Santana; Rodrigues, L. R.; Cerqueira, Nuno M. F. S. A.; Oliveira‐Campos, Ana M. F.; Rodrigues, Lígia M.; Esteves, Ana Paula

doi:10.1016/j.bmc.2013.06.049

Cited by 19 publications

(14 citation statements)

References 56 publications

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“…Furthermore, the compound 4 showed better activity for the MDA MB231 cell line than compounds 3 and 5, although for the TCC-SUP cell line it gave values on the same range as the compounds 3 and 5. The results herein obtained are in agreement with our previous studies using benzopsoralen analogues [4,5].…”

Section: Anti-proliferative Effect On Human Cancer Cell Linessupporting

confidence: 93%

“…Therefore, it is an adequate model for molecular docking studies of the compounds herein synthesized. Previously, we reported that these compounds interact very closely with the iron ion of the haem group of the enzyme [4,5]. Ye and Zhang [16] demonstrated that the depletion of iron (haem deficiency) caused the apoptosis of HeLa cells, which involved the release of cytochrome c and the activation of caspase 3 (involved in the programmed cell death).…”

Section: Introductionmentioning

confidence: 98%

“…Additionally, Psoralen and 8-methoxypsoralen (8-MOP, named Xanthotoxin) are used for the treatment of Psoriasis in combination with UVA irradiation (PUVA therapy) [3]. It is important to notice that these compounds have also been reported to have an anti-cancer effect independently of its photoactivation [4,5]. It has been reported that Bergapten (5-methoxypsoralen) enhances p53 gene expression and induces apoptosis in human breast cancer cells [6].…”

Section: Introductionmentioning

confidence: 99%

“…Earlier in our group Psoralen derivatives were synthesized and their anti-proliferative effects on different human tumour cell lines were demonstrated [4,5]. The molecular docking results of these compounds with the CYP2A6 enzyme showed that, in general, the compounds carrying few bulky groups attached to the coumarin moiety adopted a conformation that allows the carbonyl group of the coumarin moiety to interact very closely with the iron ion of the haem cluster.…”

Section: Introductionmentioning

confidence: 99%

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Novel benzopsoralen analogues: Synthesis, biological activity and molecular docking studies

Francisco

Rodrigues

Cerqueira

et al. 2014

European Journal of Medicinal Chemistry

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New benzopsoralen analogues were synthesized and their inhibitory effect on the growth of tumourtumour cell lines (MDA MB231 and TCC-SUP) was evaluated. The in vitro antitumour activity of the new benzopsoralen analogues was discussed in terms of structure-activity relationship. Molecular docking studies with human-CYP2A6 enzymes were also carried out with the synthesized compounds to evaluate the potential of these molecules to interact with the haem group of the enzymes. The results demonstrated that the compounds that are able to interact with the iron ion of the haem cofactor and at the same time with active site Asn297 are those that have better anti-proliferative activity.

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Section: Anti-proliferative Effect On Human Cancer Cell Linessupporting

confidence: 93%

Section: Introductionmentioning

confidence: 98%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Novel benzopsoralen analogues: Synthesis, biological activity and molecular docking studies

Francisco

Rodrigues

Cerqueira

et al. 2014

European Journal of Medicinal Chemistry

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“…As shown in Scheme 4, the tert-butyl and methyl groupso f4a were easily removed by AlCl 3 in refluxing toluene, affording dibenzofuran-2-ol 7 in 91 %y ield. Compound 7 is an important intermediate for the synthesis of many bioactive substances, such as HeLa (cervix adenocarcinoma) and TCC-SUP (bladder transitional cell carcinoma) cells inhibitor 8, [20] HeLa and MDA MB231 (breasta denocarcinoma) cells inhibitor 9, [21] and H37Rv (mycobacterium tuberculosis) growth inhibitor 10. [22] In summary,an ovel coppercatalyzed tandemo xidative homocoupling/skeletal rearrangement of phenolst hat involves the cleavage of ab enzene ring under mild reaction conditions has been realized by using air or Ag 2 CO 3 as the oxidant.…”

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confidence: 99%

Oxidant‐Controlled Catalytic Transformations of Phenols with Unexpected Cleavage of Aromatic Rings

Song

You

2015

Chemistry A European J

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Oxidative transformations of phenols have attracted significant attention of chemists due to their importance in biological process and organic synthesis. In contrast to the relatively well-developed oxygenation and coupling reactions of phenols, the highly efficient and selective oxidative ring cleavage of phenols is under-represented. This work describes a novel CuCl-catalyzed tandem homocoupling/skeletal rearrangement of phenols that realizes the cleavage of the phenol ring by using air or Ag2CO3 as the oxidant. Interestingly, simply changing the oxidant to K2S2O8 results in the oxidative coupling/cyclization of phenols to give dibenzofurans. These results set an important precedent of oxidant-controlled catalytic transformations of phenols.

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Annulated Heterocyclic[g]Coumarin Composites: Synthetic Approaches and Bioactive Profiling

Mazin Zeki,

Fakri Mustafa

2024

Chemistry & Biodiversity

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Coumarins, widely abundant natural heterocyclic compounds, are extensively employed in creating various biologically and pharmacologically potent substances. The hybridization of heterocycles presents a key opportunity to craft innovative multicyclic compounds with enhanced biological activity. Fusing different heterocyclic rings with the coumarin structure presents an intriguing method for crafting fresh hybrid compounds possessing remarkable biological effects. In the pursuit of creating heterocyclic‐fused coumarins, a wide range of annulated heterocyclic[g]coumarin composites has been introduced, displaying impressive biological potency. The influence of the linear attachment of heterocyclic rings to the coumarin structure on the biological performance of the resulting compounds has been investigated. This review centers on the synthetic methodologies, structural activity relationship investigation, and biological potentials of annulated heterocyclic[g]coumarin composites. We conducted searches across several databases, including Web of Science, Google Scholar, PubMed, and Scopus. After sieving, we ultimately identified and included 71 pertinent studies published between 2000 and the middle of 2023. This will provide valuable perspectives for medicinal chemists in the prospective design and synthesis of lead compounds with significant therapeutic effects, centered around heterocycle‐fused coumarin frameworks.

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Synthesis of novel psoralen analogues and their in vitro antitumor activity

Cited by 19 publications

References 56 publications

Novel benzopsoralen analogues: Synthesis, biological activity and molecular docking studies

Novel benzopsoralen analogues: Synthesis, biological activity and molecular docking studies

Oxidant‐Controlled Catalytic Transformations of Phenols with Unexpected Cleavage of Aromatic Rings

Annulated Heterocyclic[g]Coumarin Composites: Synthetic Approaches and Bioactive Profiling

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