Antiproliferative Activity and Effect on GABAA Receptors of Callitrisic Acid Derivatives

Stadler, Marco; Padrón, José M.; González-Cardenete, Miguel A.

doi:10.1055/s-0043-119889

Cited by 4 publications

(16 citation statements)

References 16 publications

(28 reference statements)

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“…was ester ≥ alcohol > acid, which is a trend similar to that of C19 callitrisic-derivative series. 22 Previous reports on the antiproliferative activity of sugiol β-amino alcohols analogues (6a, Figure 1), 14 provided similar cytotoxicity results against A2780, WiDr and SW1573 cancer cells after 48 h of exposure using the sulforhodamine B (SRB) assay. 14 An important difference in the β-amino alcohols analogues is the presence of a gem-dimethyl group at C4 in contrast with the C18-functionalized position in the current study.…”

Section: Chemistrysupporting

confidence: 63%

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Synthesis and Biological Studies of (+)-Liquiditerpenoic Acid A (Abietopinoic Acid) and Representative Analogues: SAR Studies

et al. 2019

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similar chemistry. The combined findings indicate that these abietane-diterpenoid natural product analogues offer a source of novel bioactive molecules with promising pharmacological and drug-likeness properties. ASSOCIATED CONTENT Supporting Information Available: Complete experimental details for the synthesis of compounds 7 and 9-16, including copies of 1 H NMR and 13 C NMR spectra, and for all the biological assays. A list with the complete results of the docking studies carried out on the analyzed targets and SMILES codes is also available in the S.I.

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Section: Chemistrysupporting

confidence: 63%

“…Most of the compounds were active (GI50 < 25 µΜ) in the solid tumor cells with higher activity than the parent dehydroabietic acid (2) from previous results. 22 The target molecule, (+)-liquiditerpenoic acid (7, Compound 9 was also more potent against T-47D and WiDr cell lines than the standard of care drug, cisplatin.…”

Section: Chemistrymentioning

confidence: 99%

Synthesis and Biological Studies of (+)-Liquiditerpenoic Acid A (Abietopinoic Acid) and Representative Analogues: SAR Studies

et al. 2019

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“…The anticancer drugs cisplatin and etoposide were used for reference. Most of the molecules were active (GI50 < 25 μM) in the solid tumor cells with higher activity than parent ferruginol (1) and sugiol (2) as reported by Li et al [25] for A549 cell line and compounds 10-12 better than the starting methyl callitrisate (7) comparing with previous results [26]. The target molecule, (+)-4-epi-liquiditerpenoic acid (8a), showed better activity than sugiol (2) for the A549 cell line.…”

Section: Antiproliferative Activitysupporting

confidence: 80%

Biological Profiling of Semisynthetic C19-Functionalized Ferruginol and Sugiol Analogues

et al. 2021

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The abietane-type diterpenoids are significant bioactive compounds exhibiting a varied range of pharmacological properties. In this study, the first synthesis and biological investigation of the new abietane-diterpenoid (+)-4-epi-liquiditerpenoid acid (8a) together with several of its analogs are reported. The compounds were generated from the readily available methyl callitrisate (7), which was obtained from callitrisic acid present in Moroccan Sandarac resin. A biological evaluation was conducted to determine the effects of the different functional groups present in these molecules, providing basic structure–activity relationship (SAR) elements. In particular, the ferruginol and sugiol analogs compounds 10–16 were characterized by the presence of a phenol moiety, higher oxidization states at C-7 (ketone), and the hydroxyl, methyl ester or free carboxylic acid at C19. The biological profiling of these compounds was investigated against a panel of six human solid tumor cell lines (HBL-100, A549, HeLa, T-47D, SW1573 and WiDr), four parasitic Leishmania species (L. donovani, L. infantum, L. guyanensis and L. amazonensis) and two malaria strains (3D7 and K1). Furthermore, the capacity of the compounds to modulate gamma-aminobutyric acid type A (GABAA) receptors (α1β2γ2s) is also described. A comparison of the biological results with those previously reported of the corresponding C18-functionalized analogs was conducted.

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“…Compounds 1-5 were evaluated for antiproliferative activity using the protocol of the National Cancer Institute (NCI) of the USA with minor modifications. [3][4][5] Cells were seeded onto 96-well plates at cell densities of 2,500 (A549, HBL-100, HeLa and SW1573) or 5,000 (T-47D and WiDr) cells per well, depending on their doubling times. The results, expressed as GI 50 (50% growth inhibition) values after 48 h of drug exposure, were calculated according to NCI formulas.…”

Section: Antiproliferative Assaysmentioning

confidence: 99%

“…• Phytochemical investigation of the ethanolic extract of the aerial parts of Pterocaulon alopecuroides (Asteraceae) afforded the compounds 7-(2,3-dihydroxy-3-methylbutoxy)-6-methoxycoumarin (1), 5,6-methylenedioxy-7-(2,3-dihydroxy-3-methylbutoxy) coumarin (2), Dihydrokaempferol (3), 5,7,4´-trihydroxy-6-(α,α-dimethylallyl)dihydroflavonol (4) and 5,4´-dihydroxy-7-(γ,γ-dimethylallyloxy)dihydroflavonol (5). All isolates were evaluated for their antiproliferative activities on a panel of six human tumor cell lines.…”

Section: Conflict Of Interestmentioning

confidence: 99%

Secondary Metabolites from Pterocaulon alopecuroides and their Antiproliferative Activities

Castillo¹,

Padrón²,

Emiliano³

2019

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Objective: To isolate secondary metabolites from the aerial parts of Pterocaulon alopecuroides, elucidate their structures and evaluate their antiproliferative activities on selected human cancer cell lines. Materials and Methods: The ethanolic extract of P. alopecuroides afforded five compounds, which were characterized using spectroscopic techniques and by comparison with data from the literature. Antiproliferative activities of all isolates were evaluated. Results: The compounds 7-(2,3-dihydroxy-3-methylbutoxy)-6-methoxycoumarin (1), 5,6-methylenedioxy-7-(2,3-dihydroxy-3-methylbutoxy) coumarin (2), Dihydrokaempferol (3), 5,7,4´-trihydroxy-6-(α,α-dimethylallyl)dihydroflavonol (4) and 5,4´-dihydroxy-7-(γ,γ-dimethylallyloxy)dihydroflavonol (5) were isolated. The antiproliferative activity of all compounds was evaluated in a panel of six human solid tumor cell lines showing GI 50 values for the most active compounds in the low micromolar range. Conclusion: Compound 2 is reported for first time from P. alopecuroides. Isolated coumarins show no antiproliferative activity, whilst among flavonoids compound 5 showed the best antiproliferative activity.

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Antiproliferative Activity and Effect on GABAA Receptors of Callitrisic Acid Derivatives

Cited by 4 publications

References 16 publications

Synthesis and Biological Studies of (+)-Liquiditerpenoic Acid A (Abietopinoic Acid) and Representative Analogues: SAR Studies

Synthesis and Biological Studies of (+)-Liquiditerpenoic Acid A (Abietopinoic Acid) and Representative Analogues: SAR Studies

Biological Profiling of Semisynthetic C19-Functionalized Ferruginol and Sugiol Analogues

Secondary Metabolites from Pterocaulon alopecuroides and their Antiproliferative Activities

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