<i>In Vivo</i> Effects of Vanadium Pentoxide and Antioxidants (Ascorbic Acid and Alpha‐Tocopherol) on Apoptotic, Cytotoxic, and Genotoxic Damage in Peripheral Blood of Mice

Garcia‐Rodriguez, María del Carmen; Hernández-Cortés, Lourdes Montserrat; Altamirano-Lozano, Mario

doi:10.1155/2016/6797851

Cited by 15 publications

(12 citation statements)

References 57 publications

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“…Our data also revealed that ascorbic acid was able to reduce meglumine antimoniate-induced genomic damage, corroborating previous studies that observed a protective effect of ascorbic acid against mutagenic damage induced by other stressors such as cyclophosphamide (44), arsenic trioxide (45), 3,5-dimethylaminophenol (46), and vanadium pentoxide (47). Ascorbic acid is a nonenzymatic antioxidant obtained from the diet and is essential to humans due to its participation in several physiological activities (48).…”

Section: Discussionsupporting

confidence: 91%

Genistein and Ascorbic Acid Reduce Oxidative Stress-Derived DNA Damage Induced by the Antileishmanial Meglumine Antimoniate

Jesus

Soares

Moreira

et al. 2018

Antimicrob Agents Chemother

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Meglumine antimoniate (Glucantime) is a pentavalent antimonial used to treat leishmaniasis, despite its acknowledged toxic effects, such as its ability to cause oxidative damage to lipids and proteins. Recently, our group demonstrated that meglumine antimoniate causes oxidative stress-derived DNA damage. Knowing that antioxidants modulate reactive oxygen species, we evaluated the capacity of genistein and ascorbic acid for preventing genotoxicity caused by meglumine antimoniate. For that, mice (n= 5/group) received genistein (via gavage) in doses of 5, 10, and 20 mg/kg for three consecutive days. After this period, they were treated with 810 mg/kg meglumine antimoniate via intraperitoneal (i.p.) route. Furthermore, mice (n= 5/group) simultaneously received ascorbic acid (i.p.) in doses of 30, 60, and 120 mg/kg and 810 mg/kg meglumine antimoniate. We also conducted post- and pretreatment assays, in which animals received ascorbic acid (60 mg/kg) 24 h prior to or after receiving meglumine antimoniate. Genomic instability and mutagenicity were analyzed through conventional comet assay and enzymatic assay using formamide pyrimidine DNA glycosylase (Fpg) enzyme, as well as the micronucleus test, respectively. Meglumine antimoniate induced an increase in the DNA damage after digestion with Fpg, reinforcing its mutagenic potential by oxidizing DNA bases, which was prevented by genistein. Similarly, ascorbic acid was capable of reducing mutagenic effects in simultaneous treatment as well as in posttreatment. Therefore, our results demonstrate that both compounds are efficient in preventing mutations in mammalian cells treated with meglumine antimoniate.

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Section: Discussionsupporting

confidence: 91%

Genistein and Ascorbic Acid Reduce Oxidative Stress-Derived DNA Damage Induced by the Antileishmanial Meglumine Antimoniate

Jesus

Soares

Moreira

et al. 2018

Antimicrob Agents Chemother

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“…Therefore, it has been proposed that the chemopreventive properties of antioxidants are related to their ability to target speciic cellular signaling pathways that regulate cellular proliferation and apoptosis [43]. This proposal is consistent with our results since the frequencies of apoptotic cells (particularly, late apoptotic cells) indeed increased signiicantly with the administration of vitamin C, and their administration prior to treatment of V 2 O 5 increased them even further [8]. Additionally, other studies have reported that the apoptosis-inducing activity of antioxidants might be synergistically enhanced by a combined treatment with chemopreventive [44] or genotoxic agents [40].…”

Section: Protective Efects Of Vitamin C Against Genotoxic Damage Fromsupporting

confidence: 91%

“…Additionally, the promising low costs of vanadium-based drugs make it particularly atractive, and the ability to overcome the adverse efects of vanadium compounds during therapeutic action is an urgent and crucial issue for its future use in medicine [49]. Our indings strongly suggest that vitamin C can be used efectively in therapy either alone (antioxidant) or in combination with other agents such as V 2 O 5 to reduce their genotoxicity [8].…”

Section: Protective Efects Of Vitamin C Against Genotoxic Damage Frommentioning

confidence: 90%

“…In a previous study, we observed that the frequency of micronuclei in polychromatic erythrocytes (MN-PCE) increased with the administration of 40 mg/kg of V 2 O 5 through ip [8], consistent with other studies testing soluble vanadium compounds (Na 3 VO 4 , SVO 5, and NH 4 VO 3 ) [34][35][36]. However, the in vivo administration of vitamin C prior to the V 2 O 5 injection decreased MN-PCE formation compared to administering V 2 O 5 alone, reducing basal MN-PCE, and presenting the strongest protection against genotoxic damage induced by V 2 O 5 .…”

Section: Protective Efects Of Vitamin C Against Genotoxic Damage Frommentioning

confidence: 96%

“…However, these efects can be inluenced by the action of low molecular weight antioxidants such as vitamin C, which is capable of chelating metal ions, reducing their catalytic activity, and resulting ROS formation. Since the genotoxicity of heavy metals associated with oxidative stress is based on the oxidative mechanism during reduction [5], vitamin C can be used efectively to protect or reduce the induced genotoxic efects by suppressing oxidative stress caused by these metallic compounds [6][7][8]. However, paradoxically under certain conditions (i.e., low concentration in vitro and the presence of metal ions), vitamin C can exert a pro-oxidant efect, increasing oxidative damage to lipids, DNA and protein, besides being a potential direct or indirect modulator of gene expression [9].…”

Section: Introductionmentioning

confidence: 99%

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The Role of Vitamin C in the Protection and Modulation of Genotoxic Damage Induced by Metals Associated with Oxidative Stress

2017

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This chapter reviews the efects of vitamin C on metal-induced genotoxicity. By focusing on cuting-edge studies, including our own results in experiments with vanadium(V) and chromium(VI), the suggestion that vitamin C can be used efectively to protect against or reduce the genotoxic efects induced by metal exposure by suppressing oxidative stress is particularly explored. After explaining the chemical mechanisms involved in oxidative stress associated with heavy metals, this chapter discusses the various proposals regarding the physiological processes of vitamin C at the molecular level, its relationship with oxidative stress, levels of 8-hydroxydeoxyguanosine 7, and apoptosis, and its role in the protection and modulation of DNA damage, as well as how they it with our own results that showed an increase in apoptosis and 8-OH-dG when vitamin C was administered in addition to the metallic compounds. The relevant gaps in our understanding of the role of vitamin C with regard to these issues are highlighted, as well as the key importance of its clinical use, and ultimately, human health.

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Effects of co-administration of arsenic trioxide and Schiff base oxovanadium complex on the induction of apoptosis in acute promyelocytic leukemia cells

2021

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In Vivo Effects of Vanadium Pentoxide and Antioxidants (Ascorbic Acid and Alpha‐Tocopherol) on Apoptotic, Cytotoxic, and Genotoxic Damage in Peripheral Blood of Mice

Cited by 15 publications

References 57 publications

Genistein and Ascorbic Acid Reduce Oxidative Stress-Derived DNA Damage Induced by the Antileishmanial Meglumine Antimoniate

Genistein and Ascorbic Acid Reduce Oxidative Stress-Derived DNA Damage Induced by the Antileishmanial Meglumine Antimoniate

The Role of Vitamin C in the Protection and Modulation of Genotoxic Damage Induced by Metals Associated with Oxidative Stress

Effects of co-administration of arsenic trioxide and Schiff base oxovanadium complex on the induction of apoptosis in acute promyelocytic leukemia cells

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