Publications by authors named "Elisa Valletta"

Article Synopsis
  • * Researchers analyzed blood samples from 121 children with moderate-to-severe asthma to find DNAm markers linked to BDR and FeNO, using regression models to ensure accuracy while controlling for variables like age and sex.
  • * They identified specific DNA markers and differential regions related to FeNO and BDR, with findings indicating associations with allergic reactions and inflammation, potentially opening avenues for better understanding and management of asthma in pediatric patients.
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  • Glutathione (GSH) reduces the effectiveness of cisplatin, a chemotherapy drug, in human leukaemia and ovarian cancer cells, but the addition of a copper complex [Cu(phen)(OH)](ClO) restores sensitivity to cisplatin.
  • The combination of the copper complex, cisplatin, and GSH results in a stronger toxic effect on leukaemia cells compared to healthy lymphocytes, suggesting that cancer cells are more vulnerable to this treatment.
  • Treatment with the copper complex and cisplatin triggers early and late apoptotic processes in cancer cells, indicating a strong interaction between these drugs in inducing programmed cell death without harming the cell membrane.
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Rationale: Development of therapy-resistant cancer is a major problem in clinical oncology, and there is an urgent need for novel markers identifying development of the resistant phenotype. Lipidomics represents a promising approach to discriminate lipid profiles of malignant phenotype cells. Alterations in phospholipid distribution or chemical composition have been reported in various pathologies including cancer.

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Coumarins show biological activity and are widely exploited for their therapeutic effects. Although a great number of coumarins substituted by heterocyclic moieties have been prepared, few studies have been carried out on coumarins containing pyridine heterocycle, which is known to modulate their physiological activities. We prepared and characterized three novel 3-(pyridin-2-yl)coumarins and their corresponding copper(II) complexes.

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  • Cisplatin (CDDP) is a common cancer treatment, but its effectiveness is often reduced due to patient resistance linked to high levels of glutathione (GSH), which can deactivate the drug.
  • Studies show that combining CDDP with the copper complex [Cu(phen)(HO)](ClO) can restore sensitivity in cisplatin-resistant leukemic and ovarian cancer cells.
  • Research indicates that while CDDP can react with GSH and copper compounds, in mixtures involving CDDP and copper complexes, only copper-glutathione complexes were found, not platinum-glutathione adducts.
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Cross-contamination of eukaryotic cell lines used in biomedical research represents a highly relevant problem. Analysis of repetitive DNA sequences, such as Short Tandem Repeats (STR), or Simple Sequence Repeats (SSR), is a widely accepted, simple, and commercially available technique to authenticate cell lines. However, it provides only qualitative information that depends on the extent of reference databases for interpretation.

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The speciation of the potential antitumor agent vanadocene dichloride ([Cp2VCl2], abbreviated with VDC) in the blood plasma was studied by instrumental (EPR, ESI-MS, MS-MS, and electronic absorption spectroscopy) and computational (DFT) methods. The behavior of VDC at pH 7.4 in aqueous solution, the interaction with the most important bioligands of the plasma (oxalate, carbonate, phosphate, lactate, citrate, histidine, and glycine among those with low molecular mass and transferrin and albumin between the proteins) was evaluated.

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Cisplatin, cis-diammineplatinum(II) dichloride, is a metal complex used in clinical practice for the treatment of cancer. Despite its great efficacy, it causes adverse reactions and most patients develop a resistance to cisplatin. To overcome these issues, a multi-drug therapy was introduced as a modern approach to exploit the drug synergy.

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The tetrahedral S-coordinated complex [Zn(MeImHS)4](ClO4)2, synthesised from the reaction of [Zn(ClO4)2] with methimazole (1-methyl-3H-imidazole-2-thione, MeImHS), reacts with triethylamine to yield the homoleptic complex [Zn(MeImS)2] (MeImS = anion methimazole). ESI-MS and MAS (13)C-NMR experiments supported MeImS acting as a (N,S)-chelating ligand. The DFT-optimised structure of [Zn(MeImS)2] is also reported and the main bond lengths compared to those of related Zn-methimazole complexes.

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The cytotoxic properties of copper(II) complexes with 1,10-phenanthroline (phen) can be modified by substitution in the phen backbone. For this purpose, Cu(II) complexes with phen, 1,10-phenanthrolin-5,6-dione (phendione) and 1,10-phenanthrolin-5,6-diol (phendiol) have been synthesised and characterised. The crystal structure of [Cu(phendione)2(OH2)(OClO3)](ClO4) is discussed.

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