Kinetic Studies of Sodium and Metforminium Decavanadates Decomposition and In Vitro Cytotoxicity and Insulin- Like Activity

Nolasco, Aniela M. Silva; Camacho, Luz; Dı́az, Rosalinda; Abreu, Oswaldo Hernández; León, Ignacio E.; Lombardo, Irma Sánchez

doi:10.3390/inorganics8120067

Cited by 15 publications

(20 citation statements)

References 70 publications

(117 reference statements)

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“…It is very important to note that for the determination of the IC 50 values and the type of inhibition described above, the Metf-V 10 compound was added to the medium immediately before the beginning of the reaction being the rate measure within the next 2-3 min. The kinetics of the decomposition reaction of V 10 as well as of Metf-V 10 was previously determined by UV/Vis and 51 V NMR spectroscopy [45,66]. It was described that after addition of V 10 and/or Metf-V 10 in the medium, intact V 10 species with amounts of vanadate oligomers were detected [21,45,66].…”

Section: Discussionmentioning

confidence: 99%

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Decavanadate and metformin-decavanadate effects in human melanoma cells

Sousa‐Coelho

Aureliano

Fraqueza

et al. 2022

Journal of Inorganic Biochemistry

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Section: Discussionmentioning

confidence: 99%

“…The Metf-V 10 crystals were solubilized in 10% dimethyl sulfoxide (DMSO) to a 5 mM stock concentration. Such vanadium compounds were previously characterized [40,[43][44][45].…”

Section: Preparation Of Decavanadate and Metformin-decavanadatementioning

confidence: 99%

Decavanadate and metformin-decavanadate effects in human melanoma cells

Sousa‐Coelho

Aureliano

Fraqueza

et al. 2022

Journal of Inorganic Biochemistry

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“…Recently, a study reported the upregulation of hepatic AMPK levels and Akt cascade by a synergistic combination of metformin and bis(α-furancarboxylato)oxovanadium(IV) (BFOV) for the treatment of fatty liver disease [161]. Such reports of synergistic action of metformin and vanadium salts are not uncommon [162]. The most extensively studied vanadium compound in this context is vanadium(IV)chlorodipicolinate.…”

Section: Vanadium-mediated Ampk Activation-reduced Adipogenesismentioning

confidence: 99%

Targeting Breast Cancer and Their Stem Cell Population through AMPK Activation: Novel Insights

Uprety

Abrahamse

2022

Cells

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Despite some significant advancements, breast cancer has become the most prevalent cancer in the world. One of the main reasons for failure in treatment and metastasis has been attributed to the presence of cancer initiating cells—cancer stem cells. Consequently, research is now being focussed on targeting cancer cells along with their stem cell population. Non-oncology drugs are gaining increasing attention for their potent anticancer activities. Metformin, a drug commonly used to treat type 2 diabetes, is the best example in this regard. It exerts its therapeutic action by activating 5′ adenosine monophosphate-activated protein kinase (AMPK). Activated AMPK subsequently phosphorylates and targets several cellular pathways involved in cell growth and proliferation and the maintenance of stem-like properties of cancer stem cells. Therefore, AMPK is emerging as a target of choice for developing effective anticancer drugs. Vanadium compounds are well-known PTP inhibitors and AMPK activators. They find extensive applications in treatment of diabetes and obesity via PTP1B inhibition and AMPK-mediated inhibition of adipogenesis. However, their role in targeting cancer stem cells has not been explored yet. This review is an attempt to establish the applications of insulin mimetic vanadium compounds for the treatment of breast cancer by AMPK activation and PTP1B inhibition pathways.

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“…Decavanadate’s high negative charge allows it to interact with a wide range of molecules, including proteins, counterions, and lipid structures, influencing a variety of biological processes such as muscle contraction, calcium homeostasis, necrosis, actin polymerization, oxidative stress markers, and glucose uptake ( Aureliano, 2009 ). As a result, numerous compounds based on decavanadate and cationic organic ligands have been published in recent years, which have been shown to lower blood sugar levels ( Garcia-Vicente et al, 2007 ; Treviño et al, 2015 ; Treviño et al, 2018 ; Treviño and González-Vergara, 2019 ), induce neuronal and cognitive restoration mechanisms while treating metabolic syndrome ( Diaz et al, 2021 ), and inhibit the growth of protozoan parasites ( Li et al, 2010 ; Silva-Nolasco et al, 2020 ). The cytotoxic or differentiating activity of oxidovanadium complexes with organic ligands against various cancer cell types is well known ( Kioseoglou et al, 2015 ; Crans et al, 2018 ; Crans et al, 2019 ; Redher, 2020 ; Samart et al, 2020 ; Macedo Alves de Lima et al, 2021 ; Pessoa et al, 2021 ).…”

Section: Introductionmentioning

confidence: 99%

“…As a result, studying the cyclo-tetravanadate anion is critical because it will be the dominant species at physiological pH ( Sanchez-Lara et al, 2018 ). Anticancer properties of vanadium(V) anionic compounds have been discovered ( Cheng et al, 2018 ; Silva-Nolasco et al, 2020 ). Mg(H 2 O) 6 (C 4 N 2 H7) 4 V 10 O 28 •4H 2 O and (C 7 H 10 N) 4 [H 2 V 10 O 28 ]•2H 2 O were recently shown to have dose-dependent antiproliferative activity against human cancer cells U87, IGR39, and MDA-MB-231 ( Ksiksi et al, 2021 ; Louati et al, 2021 ).…”

Section: Introductionmentioning

confidence: 99%

Tris(2-Pyridylmethylamine)V(O)2 Complexes as Counter Ions of Diprotonated Decavanadate Anion: Potential Antineoplastic Activity

et al. 2022

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The synthesis and theoretical-experimental characterization of a novel diprotanated decavanadate is presented here due to our search for novel anticancer metallodrugs. Tris(2-pyridylmethyl)amine (TPMA), which is also known to have anticancer activity in osteosarcoma cell lines, was introduced as a possible cationic species that could act as a counterpart for the decavanadate anion. However, the isolated compound contains the previously reported vanadium (V) dioxido-tpma moieties, and the decavanadate anion appears to be diprotonated. The structural characterization of the compound was performed by infrared spectroscopy and single-crystal X-ray diffraction. In addition, DFT calculations were used to analyze the reactive sites involved in the donor-acceptor interactions from the molecular electrostatic potential maps. The level of theory mPW1PW91/6–31G(d)-LANL2DZ and ECP = LANL2DZ for the V atom was used. These insights about the compounds’ main interactions were supported by analyzing the noncovalent interactions utilizing the AIM and Hirshfeld surfaces approach. Molecular docking studies with small RNA fragments were used to assess the hypothesis that decavanadate’s anticancer activity could be attributed to its interaction with lncRNA molecules. Thus, a combination of three potentially beneficial components could be evaluated in various cancer cell lines.

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Kinetic Studies of Sodium and Metforminium Decavanadates Decomposition and In Vitro Cytotoxicity and Insulin- Like Activity

Cited by 15 publications

References 70 publications

Decavanadate and metformin-decavanadate effects in human melanoma cells

Decavanadate and metformin-decavanadate effects in human melanoma cells

Targeting Breast Cancer and Their Stem Cell Population through AMPK Activation: Novel Insights

Tris(2-Pyridylmethylamine)V(O)2 Complexes as Counter Ions of Diprotonated Decavanadate Anion: Potential Antineoplastic Activity

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