Intercalation processes of copper complexes in DNA

Galindo‐Murillo, Rodrigo; García‐Ramos, Juan Carlos; Ruíz-Azuara, Lena; Cheatham, Thomas E.; Cortés‐Guzmán, Fernando

doi:10.1093/nar/gkv467

Cited by 154 publications

(105 citation statements)

References 77 publications

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“…So copper complexes are regarded as one of the most promising alternatives to cisplatin as anticancer substances. Copper complexes called Casiopeínas have proved their significant anticancer activity, both in preclinical in vitro and in vivo testing, and two of them have entered Phase I of the clinical trials . Zuo et al have reported two amino acid Schiff‐base copper complexes, which could inhibit the chymotrypsin‐like activity of 20S proteasome, cause accumulation of proteasome target proteins bax and IκB‐α, and induce growth inhibition and apoptosis in MDA‐MB‐231, MCF‐7, and PC‐3 tumor cells.…”

Section: Introductionmentioning

confidence: 99%

Retracted: Studies of proteasome inhibition and antitumor activity by novel amino acid‐polypyridine‐copper complexes

Yang

Zhao

et al. 2019

Journal of Heterocyclic Chem

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Five innovative ternary copper (II) complexes [Cu (OH‐PIP)(Phe)Cl](1), [Cu (OH‐PIP)(Gly)(H2O)]NO3·2H2O (2), [Cu (OH‐PIP)(Ala)(Cl)]·H2O (3), [Cu (OH‐PIP)(Met)]PF6·2H2O (4), and [Cu (OH‐PIP)(Gln)(H2O)]Cl·3H2O (5) have been synthesized and characterized by infrared spectroscopy, elemental analysis, and single crystal X‐ray diffraction analysis. X‐ray crystallography showed that all Cu atoms were five‐coordinated in a square‐pyramidal configuration. They are screened for in vitro cytotoxicity against a panel of human cancer cell lines CAL‐51, MDA‐MB‐231, HeLa, MCF‐7, SGC‐7901, A549, K562, and SMMC‐7721. The most promising results were achieved for complexes 1 to 5, with the IC50 values in the range of 0.082μM to 0.69μM (against CAL‐51 cell lines). The anticancer activities against CAL‐51, MDA‐MB‐231, and MCF‐7 were higher than that of Carboplatin. The mechanism studies showed that complexes 1 to 5 could inhibit proteasome activity, induce apoptosis, and inhibit cell proliferation, indicating their great potential as proteasome inhibitors for triple‐negative breast cancer therapy.

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Section: Introductionmentioning

confidence: 99%

Retracted: Studies of proteasome inhibition and antitumor activity by novel amino acid‐polypyridine‐copper complexes

Yang

Zhao

et al. 2019

Journal of Heterocyclic Chem

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“…All geometrical optimizations were carried out at the DFT (B3LYP) [58,59] level of theory with 6-31+G* basis set for C, N, O, S, Cl, Br, H and DZpdf [60] for the copper center using Gaussian 09 program [61]. In order to check the binding modes of the copper nucleases, three DNA sequences were used in the verified docking studies: d(5'-ATATATATATAT-3')2 (assigned as DNA1) which is AT-rich sequence, d(5'-CGCGCGCGCGCG-3')2 (assigned as DNA2) which is GC-rich sequence and d(5'-CGCGAATTCGCG-3')2 (assigned as DNA3) which not only contains AT base pair but also contains CG one and is mostly used in molecular docking studies [62][63][64][65]. Three DNAs adopted in this study are B-DNA , which were built by 3DNA [66].…”

Section: Initial Structuresmentioning

confidence: 99%

“…Even though experimental results have demonstrated the DNAcleavage activity of some copper nucleases, the investigations of nuclease-DNA binding modes and cleavage mechanisms of DNA by copper nucleases at the molecular level remain limited. The theoretical approaches provide a powerful tool to evaluate the metal-based compounds interactions with DNA [26][27][28][29][30][31][32][33][34][35]. To the best of our understanding, in the light of available information, the mechanism of nuclease-DNA binding and its effect on DNA secondary structure have not been comprehensively studied in a systematic manner.…”

Section: Introductionmentioning

confidence: 99%

Theoretical studies on binding modes of copper-based nucleases with DNA

Liu

Zhu

Tang

2016

Journal of Molecular Graphics and Modelling

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“…Thus, copper complexes are regarded as some of the most promising metal alternatives to platinum compounds in cancer treatment . Copper complexes called Casiopeínas ® have proved their anticancer activity in both preclinical in vitro and in vivo testing, and two of them have entered Phase I clinical trials . Zuo et al .…”

Section: Introductionmentioning

confidence: 99%

Studies of proteasome inhibition and apoptosis induction in triple‐negative breast cancer cells by novel amino acid–polypyridine–copper complex

Wang

Yagüe

et al. 2019

Applied Organom Chemis

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An innovative ternary copper(II) complex, [Cu(Cl‐PIP)(Tyr)Cl]n, has been synthesized and characterized using infrared spectroscopy, elemental analysis and single‐crystal X‐ray diffraction analysis. X‐ray crystallography indicates that the Cu atom is five‐coordinated in a square‐pyramidal configuration. The unit forms a one‐dimensional chain along the crystallographic c‐axis. The complex was screened for cytotoxicity against a panel of eight human cancer cell lines, namely MDA‐MB‐231, CAL‐51, K562, HeLa, SGC‐7901, A549, MCF‐7 and SMMC‐7721. The best anticancer activity was obtained with triple‐negative breast cancer CAL‐51 and MDA‐MB‐231 cell lines, with IC50 values in the range 0.035–0.10 μM, and this was better than using carboplatin. The complex inhibits proteasomal chymotrypsin‐like activity, and docking studies reveal its interaction with 20S proteasome. In addition, the complex causes accumulation of ubiquitinated proteins, induces apoptosis and inhibits cell proliferation, indicating its great potential as a novel therapy for triple‐negative breast cancer.

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Intercalation processes of copper complexes in DNA

Cited by 154 publications

References 77 publications

Retracted: Studies of proteasome inhibition and antitumor activity by novel amino acid‐polypyridine‐copper complexes

Retracted: Studies of proteasome inhibition and antitumor activity by novel amino acid‐polypyridine‐copper complexes

Theoretical studies on binding modes of copper-based nucleases with DNA

Studies of proteasome inhibition and apoptosis induction in triple‐negative breast cancer cells by novel amino acid–polypyridine–copper complex

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