Your search keyword '"Cordelli E"' showing total 26 results

1. Pyrogenic synthetic amorphous silica (NM-203): Genotoxicity in rats following sub-chronic oral exposure.

Author

Villani P, Eleuteri P, Pacchierotti F, Maranghi F, Tassinari R, Narciso L, Tait S, Lori G, Andreoli C, Huet S, Jarry G, Fessard V, and Cordelli E

Subjects

Animals, Comet Assay, Female, Male, Micronucleus Tests, Rats, Rats, Sprague-Dawley, DNA Damage, Silicon Dioxide toxicity

Abstract

The genotoxicity of nano-structured synthetic amorphous silica (SAS), a common food additive, was investigated in vivo in rats. A 90-day oral toxicity study was performed according to OECD test guideline 408 and the genotoxicity of pyrogenic SAS nanomaterial NM-203 was assessed in several organs, using complementary tests. Adult Sprague-Dawley rats of both sexes were treated orally for 90 days with 0, 2, 5, 10, 20, or 50 mg SAS/kg bw per day. Dose levels were selected to approximate expected human dietary exposures to SAS. DNA strand breaks were evaluated by the comet assay in blood, bone marrow, liver, and spleen according to OECD test guideline 489; mutations induced in bone marrow precursors of erythrocytes were assessed by the Pig-a assay and chromosome/ genome damage by the micronucleus assay in blood (OECD test guideline 474) and colon. No treatment-related increases of gene (Pig-a) or chromosome/genome (micronucleus) mutations were detected in the blood. The percentage of micronucleated cells was not increased in the colon of treated rats. Among the organs analyzed by the comet assay, the spleen was the only target showing a weak but biologically relevant genotoxic effect., (Copyright © 2022 Elsevier B.V. All rights reserved.)

Published

2022

2. Clinical and genomic safety of treatment with Ginkgo biloba L. leaf extract (IDN 5933/Ginkgoselect®Plus) in elderly: a randomised placebo-controlled clinical trial [GiBiEx].

Author

Bonassi S, Prinzi G, Lamonaca P, Russo P, Paximadas I, Rasoni G, Rossi R, Ruggi M, Malandrino S, Sánchez-Flores M, Valdiglesias V, Benassi B, Pacchierotti F, Villani P, Panatta M, and Cordelli E

Subjects

Aged, Aged, 80 and over, Female, Genome drug effects, Humans, Liver drug effects, Liver Function Tests, Male, Micronucleus Tests, DNA Damage drug effects, Ginkgo biloba chemistry, Plant Extracts administration & dosage, Plant Extracts adverse effects, Plant Extracts pharmacology, Plant Leaves chemistry

Abstract

Background: Numerous health benefits have been attributed to the Ginkgo biloba leaf extract (GBLE), one of the most extensively used phytopharmaceutical drugs worldwide. Recently, concerns of the safety of the extract have been raised after a report from US National Toxicology Program (NTP) claimed high doses of GBLE increased liver and thyroid cancer incidence in mice and rats. A safety study has been designed to assess, in a population of elderly residents in nursing homes, clinical and genomic risks associated to GBLE treatment., Methods: GiBiEx is a multicentre randomized clinical trial, placebo controlled, double blinded, which compared subjects randomized to twice-daily doses of either 120-mg of IDN 5933 (also known as Ginkgoselect®Plus) or to placebo for a 6-months period. IDN 5933 is extracted from dried leaves and contains 24.3% flavone glycosides and 6.1% of terpene lactones (2.9% bilobalide, 1.38% ginkgolide A, 0.66% ginkgolide B, 1.12% ginkgolide C) as determined by HPLC. The study was completed by 47 subjects, 20 in the placebo group and 27 in the treatment group. Clinical (adverse clinical effect and liver injury) and genomic (micronucleus frequency, comet assay, c-myc, p53, and ctnnb1 expression profile in lymphocytes) endpoints were assessed at the start and at the end of the study., Results: No adverse clinical effects or increase of liver injury markers were reported in the treatment group. The frequency of micronuclei [Mean Ratio (MR) = 1.01, 95% Confidence Intervals (95% CI) 0.86-1.18), and DNA breaks (comet assay) (MR = 0.91; 95% CI 0.58-1.43), did not differ in the two study groups. No significant difference was found in the expression profile of the three genes investigated., Conclusions: None of the markers investigated revealed a higher risk in the treatment group, supporting the safety of IDN 5933 at doses prescribed and for duration of six months., Trial Registration: ClinicalTrials.gov Identifier: NCT03004508 , December 20, 2016. Trial retrospectively registered.

Published

2018

3. Cytotoxicity, genotoxicity and gene expression changes elicited by exposure of human hepatic cells to Ginkgo biloba leaf extract.

Author

Grollino MG, Raschellà G, Cordelli E, Villani P, Pieraccioli M, Paximadas I, Malandrino S, Bonassi S, and Pacchierotti F

Subjects

Cell Line, Cell Survival drug effects, Comet Assay, Ginkgo biloba chemistry, Hepatocytes cytology, Hepatocytes metabolism, Humans, Insulin-Like Growth Factor Binding Protein 3 genetics, Insulin-Like Growth Factor Binding Protein 3 metabolism, Plant Extracts chemistry, Plant Leaves chemistry, Reactive Oxygen Species metabolism, DNA Damage drug effects, Gene Expression drug effects, Ginkgo biloba toxicity, Hepatocytes drug effects, Plant Extracts toxicity

Abstract

The use of Ginkgo biloba leaf extract as nutraceutical is becoming increasingly common. As a consequence, the definition of a reliable toxicological profile is a priority for its safe utilization. Recently, contrasting data have been reported on the carcinogenic potential of Ginkgo biloba extract in rodent liver. We measured viability, Reactive Oxygen Species (ROS), apoptosis, colony-forming efficiency, genotoxicity by comet assay, and gene expression changes associated with hepato-carcinogenicity in human cells of hepatic origin (HepG2 and THLE-2) treated with different concentrations (0.0005-1.2 mg/mL) of Ginkgoselect ® Plus. Our analyses highlighted a decrease of cell viability, not due to apoptosis, after treatment with high doses of the extract, which was likely due to ROS generation by a chemical reaction between extract polyphenols and some components of the culture medium. Comet assay did not detect genotoxic effect at any extract concentration. Finally, the array analysis detected a slight decrease in the expression of only one gene (IGFBP3) in Ginkgo-treated THLE-2 cells as opposed to changes in 28 genes in Aflatoxin B1 treated-cells. In conclusion, our results did not detect any significant genotoxic or biologically relevant cytotoxic effects and gross changes in gene expression using the Ginkgo extract in the hepatic cells tested., (Copyright © 2017 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2017

4. Study of TiO2 P25 Nanoparticles Genotoxicity on Lung, Blood, and Liver Cells in Lung Overload and Non-Overload Conditions After Repeated Respiratory Exposure in Rats.

Author

Relier C, Dubreuil M, Lozano Garcìa O, Cordelli E, Mejia J, Eleuteri P, Robidel F, Loret T, Pacchierotti F, Lucas S, Lacroix G, and Trouiller B

Subjects

Animals, Cell Survival drug effects, Dose-Response Relationship, Drug, Erythrocytes pathology, Inhalation Exposure, Liver pathology, Lung pathology, Male, Mutagens pharmacokinetics, Nanoparticles chemistry, Oxidative Stress drug effects, Particle Size, Rats, Sprague-Dawley, Surface Properties, Tissue Distribution, Titanium pharmacokinetics, DNA Damage, Erythrocytes drug effects, Liver drug effects, Lung drug effects, Mutagens toxicity, Nanoparticles toxicity, Titanium toxicity

Abstract

Inhaled titanium dioxide (TiO2) nanoparticles (NPs) can have negative health effects, and have been shown to cause respiratory tract cancer in rats. Inflammation has been linked to oxidative stress, and both have been described as possible mechanisms for genotoxicity of NPs, but rarely examined side-by-side in animal studies. In the present study, a wide range of complementary endpoints have been performed to study TiO2 P25 NP-induced genotoxicity in lung overload and non-overload conditions. Additionally, lung burden, inflammation, cytotoxicity and oxidative stress have also been evaluated in order to link genotoxicity with these responses. To assess quick and delayed responses after recovery, endpoints were evaluated at two time points: 2 h and 35 days after three repeated instillations. This study confirmed the previously described lung overload threshold at approximately 200-300 cm2 of lung burden for total particle surface area lung deposition or 4.2 µl/kg for volume-based cumulative lung exposure dose, above which lung clearance is impaired and inflammation is induced. Our results went on to show that these overload doses induced delayed genotoxicity in lung, associated with persistent inflammation only at the highest dose. The lowest tested doses had no toxicity or genotoxicity effects in the lung. In blood, no lymphocyte DNA damage, erythrocytes chromosomal damage or gene mutation could be detected. Our data also demonstrated that only overload doses induced liver DNA lesions irrespective of the recovery time. Tested doses of TiO2 P25 NPs did not induce glutathione changes in lung, blood or liver at both recovery times., (© The Author 2017. Published by Oxford University Press on behalf of the Society of Toxicology. All rights reserved. For Permissions, please e-mail: journals.permissions@oup.com.)

Published

2017

5. No genotoxicity in rat blood cells upon 3- or 6-month inhalation exposure to CeO2 or BaSO4 nanomaterials.

Author

Cordelli E, Keller J, Eleuteri P, Villani P, Ma-Hock L, Schulz M, Landsiedel R, and Pacchierotti F

Subjects

Animals, Barium Sulfate pharmacology, Barium Sulfate toxicity, Cerium pharmacology, Cerium toxicity, DNA drug effects, Female, Leukocytes metabolism, Mutagenicity Tests, Nanostructures chemistry, Rats, Chromosome Aberrations chemically induced, DNA Damage, Inhalation Exposure, Leukocytes drug effects, Mutation, Nanostructures toxicity

Abstract

In the course of a 2-year combined chronic toxicity-carcinogenicity study performed according to Organisation for Economic Co-operation and Development (OECD) Test Guideline 453, systemic (blood cell) genotoxicity of two OECD representative nanomaterials, CeO 2 NM-212 and BaSO 4 upon 3- or 6-month inhalation exposure to rats was assessed. DNA effects were analysed in leukocytes using the alkaline Comet assay, gene mutations and chromosome aberrations were measured in erythrocytes using the flow cytometric Pig-a gene mutation assay and the micronucleus test (applying both microscopic and flow cytometric evaluation), respectively. Since nano-sized CeO 2 elicited lung effects at concentrations of 5mg/m 3 (burdens of 0.5mg/lung) in the preceding range-finding study, whereas nano-sized BaSO 4 did not induce any effect, female rats were exposed to aerosol concentrations of 0.1 up to 3mg/m 3 CeO 2 or 50mg/m 3 BaSO 4 nanomaterials (6h/day; 5 days/week; whole-body exposure). The blood of animals treated with clean air served as negative control, whereas blood samples from rats treated orally with three doses of 20mg/kg body weight ethylnitrosourea at 24h intervals were used as positive controls. As expected, ethylnitrosourea elicited significant genotoxicity in the alkaline Comet and Pig-a gene mutation assays and in the micronucleus test. By contrast, 3- and 6-month CeO 2 or BaSO 4 nanomaterial inhalation exposure did not elicit significant findings in any of the genotoxicity tests. The results demonstrate that subchronic inhalation exposure to different low doses of CeO 2 or to a high dose of BaSO 4 nanomaterials does not induce genotoxicity on the rat hematopoietic system at the DNA, gene or chromosome levels., (© The Author 2016. Published by Oxford University Press on behalf of the UK Environmental Mutagen Society. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2017

6. Genotoxicity Induced by Foetal and Infant Exposure to Magnetic Fields and Modulation of Ionising Radiation Effects.

Author

Udroiu I, Antoccia A, Tanzarella C, Giuliani L, Pacchierotti F, Cordelli E, Eleuteri P, Villani P, and Sgura A

Subjects

Animals, Cell Differentiation radiation effects, Cell Proliferation radiation effects, Female, Germ Cells radiation effects, Mice, Pregnancy, DNA Damage radiation effects, Embryonic Development radiation effects, Magnetic Fields adverse effects, Prenatal Exposure Delayed Effects, Radiation, Ionizing

Abstract

Background: Few studies have investigated the toxicity and genotoxicity of extremely low frequency magnetic fields (ELF-MF) during prenatal and neonatal development. These phases of life are characterized by cell proliferation and differentiation, which might make them sensitive to environmental stressors. Although in vitro evidences suggest that ELF-MF may modify the effects of ionizing radiation, no research has been conducted so far in vivo on the genotoxic effects of ELF-MF combined with X-rays., Aim and Methods: Aim of this study was to investigate in somatic and germ cells the effects of chronic ELF-MF exposure from mid gestation until weaning, and any possible modulation produced by ELF-MF exposure on ionizing radiation-induced damage. Mice were exposed to 50 Hz, 65 μT magnetic field, 24 hours/day, for a total of 30 days, starting from 12 days post-conception. Another group was irradiated with 1 Gy X-rays immediately before ELF-MF exposure, other groups were only X-irradiated or sham-exposed. Micronucleus test on blood erythrocytes was performed at multiple times from 1 to 140 days after birth. Additionally, 42 days after birth, genotoxic and cytotoxic effects on male germ cells were assessed by comet assay and flow cytometric analysis., Results: ELF-MF exposure had no teratogenic effect and did not affect survival, growth and development. The micronucleus test indicated that ELF-MF induced a slight genotoxic damage only after the maximum exposure time and that this effect faded away in the months following the end of exposure. ELF-MF had no effects on ionizing radiation (IR)-induced genotoxicity in erythrocytes. Differently, ELF-MF appeared to modulate the response of male germ cells to X-rays with an impact on proliferation/differentiation processes. These results point to the importance of tissue specificity and development on the impact of ELF-MF on the early stages of life and indicate the need of further research on the molecular mechanisms underlying ELF-MF biological effects.

Published

2015

7. X-ray induced DNA damage and repair in germ cells of PARP1(-/-) male mice.

Author

Villani P, Fresegna AM, Ranaldi R, Eleuteri P, Paris L, Pacchierotti F, and Cordelli E

Subjects

Animals, Comet Assay, Flow Cytometry, Histones, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Phosphorylation, Poly (ADP-Ribose) Polymerase-1, Poly(ADP-ribose) Polymerases genetics, DNA Damage radiation effects, DNA Repair radiation effects, Germ Cells metabolism, Germ Cells radiation effects, Poly(ADP-ribose) Polymerases metabolism, X-Rays adverse effects

Abstract

Poly(ADP-ribose)polymerase-1 (PARP1) is a nuclear protein implicated in DNA repair, recombination, replication, and chromatin remodeling. The aim of this study was to evaluate possible differences between PARP1(-/-) and wild-type mice regarding induction and repair of DNA lesions in irradiated male germ cells. Comet assay was applied to detect DNA damage in testicular cells immediately, and two hours after 4 Gy X-ray irradiation. A similar level of spontaneous and radiation-induced DNA damage was observed in PARP1(-/-) and wild-type mice. Conversely, two hours after irradiation, a significant level of residual damage was observed in PARP1(-/-) cells only. This finding was particularly evident in round spermatids. To evaluate if PARP1 had also a role in the dynamics of H2AX phosphorylation in round spermatids, in which γ-H2AX foci had been shown to persist after completion of DNA repair, we carried out a parallel analysis of γ-H2AX foci at 0.5, 2, and 48 h after irradiation in wild-type and PARP1(-/-) mice. No evidence was obtained of an effect of PARP1 depletion on H2AX phosphorylation induction and removal. Our results suggest that, in round spermatids, under the tested experimental conditions, PARP1 has a role in radiation-induced DNA damage repair rather than in long-term chromatin modifications signaled by phosphorylated H2AX.

Published

2013

8. Direct and delayed X-ray-induced DNA damage in male mouse germ cells.

Author

Cordelli E, Eleuteri P, Grollino MG, Benassi B, Blandino G, Bartoleschi C, Pardini MC, Di Caprio EV, Spanò M, Pacchierotti F, and Villani P

Subjects

Animals, DNA Repair, Male, Mice, Mice, Inbred C57BL, Mutagenicity Tests, Spermatogenesis radiation effects, Testis radiation effects, DNA Damage, Mutation radiation effects, Spermatozoa radiation effects, X-Rays adverse effects

Abstract

Sperm DNA integrity is essential for the accurate transmission of paternal genetic information. Various stages of spermatogenesis are characterized by large differences in radiosensitivity. Differentiating spermatogonia are susceptible to radiation-induced cell killing, but some of them can repair DNA damage and progress through differentiation. In this study, we applied the neutral comet assay, immunodetection of phosphorylated H2AX (γ-H2AX) and the Sperm Chromatin Structure Assay (SCSA) to detect DNA strand breaks in testicular cells and spermatozoa at different times following in vivo X-ray irradiation. Radiation produced DNA strand breaks in testicular cells that were repaired within the first few hours after exposure. Spermatozoa were resistant to the induction of DNA damage, but non-targeted DNA lesions were detected in spermatozoa derived from surviving irradiated spermatogonia. These lesions formed while round spermatids started to elongate within the testicular seminiferous tubules. The transcription of pro-apoptotic genes at this time was also enhanced, suggesting that an apoptotic-like process was involved in DNA break production. Our results suggest that proliferating spermatogonia retain a memory of the radiation insult that is recognized at a later developmental stage and activates a process leading to DNA fragmentation., (Copyright © 2012 Wiley Periodicals, Inc.)

Published

2012

9. Evaluation of a modified comet assay to detect DNA damage in mammalian sperm exposed in vitro to different mutagenic compounds.

Author

Villani P, Spanò M, Pacchierotti F, Weimer M, and Cordelli E

Subjects

Animals, Cattle, Comet Assay standards, Dose-Response Relationship, Drug, HeLa Cells, Humans, Male, Reproducibility of Results, Spermatozoa metabolism, Comet Assay methods, DNA Damage, Mutagens toxicity, Spermatozoa drug effects

Abstract

The final stages of male gametogenesis are sensitive targets of DNA-reactive chemicals, most of which form adducts. Comet assay is a widely applied genotoxicity test that reveals DNA adducts through breaks formed during repair processes. However, sperm cells are essentially devoid of repair enzymes and comet assay is poorly sensitive in detecting chemically induced DNA lesions in sperm. To overcome such limitation, in a previous paper we proposed a modified protocol for comet assay. In this work we further tested the method treating bull sperm with additional mutagens (diethylsulfate, mitomycin C, bleomycin and colchicine) in parallel with the standard comet assay. No treatment-related increase of DNA migration was ever detected with the standard protocol. A dose-dependent effect of diethylsulfate, was obtained with the modified assay. As expected, the mitotic poison colchicine resulted negative even by the modified assay. Results with the other two compounds were consistent with their mechanism of action., (Copyright 2009 Elsevier Inc. All rights reserved.)

Published

2010

10. Assessment of in vivo genotoxicity of the rodent carcinogen furan: evaluation of DNA damage and induction of micronuclei in mouse splenocytes.

Author

Leopardi P, Cordelli E, Villani P, Cremona TP, Conti L, De Luca G, and Crebelli R

Subjects

Animals, Comet Assay, Fluorescent Antibody Technique, Histones metabolism, In Situ Nick-End Labeling, Male, Mice, Micronuclei, Chromosome-Defective drug effects, Spleen cytology, Spleen drug effects, Carcinogens toxicity, DNA Damage drug effects, Furans toxicity

Abstract

In recent years, several surveys have highlighted the presence of the rodent carcinogen furan in a variety of food items. Even though the evidence of carcinogenicity of furan is unequivocal, the underlying mechanism has not been fully elucidated. In particular, the role of genotoxicity in furan carcinogenicity is still not clear, even though this information is considered pivotal for the assessment of the risk posed by the presence of low doses of furan in food. In this work, the genotoxic potential of furan in vivo has been investigated in mice, under exposure conditions similar to those associated with cancer onset in the National Toxicology Program long-term bioassay. To this aim, male B6C3F1 mice were treated by gavage for 4 weeks with 2, 4, 8 and 15 mg furan/kg b.w./day. Spleen was selected as the target organ for genotoxicity assessment, in view of the capability of quiescent splenocytes to accumulate DNA damage induced by repeat dose exposure. The induction of primary DNA damage in splenocytes was evaluated by alkaline single-cell gel electrophoresis (comet assay) and by the immunofluorescence detection of foci of phosphorylated histone H2AX (gamma-H2AX). The presence of cross-links was probed in a modified comet assay, in which cells were irradiated in vitro with gamma-rays before electrophoresis. Chromosome damage was quantitated through the detection of micronuclei in mitogen-stimulated splenocytes using the cytokinesis-block method. Micronucleus induction was also assessed with a modified protocol, using the repair inhibitor 1-beta-arabinofuranosyl-cytosine to convert single-strand breaks in micronuclei. The results obtained show a significant (P < 0.01) increase of gamma-H2AX foci in mitogen-stimulated splenocytes of mice treated with 8 and 15 mg furan/kg b.w. and a statistically significant (P < 0.001) increases of micronuclei in binucleated splenocytes cultured in vitro. Conversely, no effect of in vivo exposure to furan was observed when freshly isolated quiescent splenocytes were analysed by immunofluorescence and in comet assays, both with standard and radiation-modified protocols. These results indicate that the in vivo exposure to furan gives rise to pre-mutagenic DNA damage in resting splenocytes, which remains undetectable until it is converted in frank lesions during the S-phase upon mitogen stimulation. The resulting DNA strand breaks are visualized by the increase in gamma-H2AX foci and may originate micronuclei at the subsequent mitosis.

Published

2010

11. ReProComet: a new in vitro method to assess DNA damage in mammalian sperm.

Author

Cordelli E, Fresegna AM, D'Alessio A, Eleuteri P, Spanò M, Pacchierotti F, and Villani P

Subjects

Animals, Cattle, HeLa Cells, Humans, Male, Spermatozoa ultrastructure, Comet Assay methods, DNA Damage, Methyl Methanesulfonate toxicity, Spermatozoa drug effects

Abstract

The increasing request of chemical safety assessment demands for the validation of alternative methods to reduce the resort to animal experimentation. Methods that evaluate reproductive toxicity are among those requiring the largest use of animals. Presently, no validated in vitro alternative exists for the assessment of reproductive toxicity. Mammalian sperm are sensitive targets of DNA-reactive chemicals, which form premutagenic adducts. Here, we propose a new method based on comet assay to detect DNA damage induced by potential germ cell mutagens in bull sperm available from assisted reproduction practices. In somatic cells, chemical-induced adducts can be revealed by comet assay that detects DNA breaks produced during adduct repair. Mature sperm, however, are devoid of repair enzymes, and adducts are processed only after fertilization. For this reason, comet assay is not sensitive to detect DNA lesions induced in sperm by most chemicals. To overcome such limitation, we developed a modified comet assay based on the addition of a protein extract from HeLa cells to agarose-embedded sperm on microscopic slides. To test the method, sperm were treated in vitro with methyl methanesulfonate (MMS) or melphalan (MLP) and comet assay was conducted both with and without protein supplementation. No effect of MMS or MLP was detected without protein supplementation; on the contrary, a clear-cut dose-dependent effect was measured after addition of the cell extract. These results represent a proof of concept of a novel in vitro mutagenicity test on sperm that could offer a promising approach to complement previously validated in vivo germ cell genotoxicity assays.

Published

2007

12. Assessment of the in vivo genotoxicity of vanadate: analysis of micronuclei and DNA damage induced in mice by oral exposure.

Author

Leopardi P, Villani P, Cordelli E, Siniscalchi E, Veschetti E, and Crebelli R

Subjects

Administration, Oral, Animals, Bone Marrow Cells drug effects, Bone Marrow Cells pathology, Bone and Bones drug effects, Bone and Bones metabolism, Comet Assay, DNA analysis, Dose-Response Relationship, Drug, Drinking, Flow Cytometry, Male, Mice, Mice, Inbred Strains, Micronuclei, Chromosome-Defective chemically induced, Micronucleus Tests, Organ Size drug effects, Reticulocytes drug effects, Reticulocytes pathology, Spermatozoa drug effects, Spermatozoa pathology, Spleen drug effects, Spleen pathology, Testis drug effects, Testis pathology, Vanadates pharmacokinetics, Vanadium analysis, Vanadium metabolism, Water Supply, DNA drug effects, DNA Damage, Mutagens toxicity, Vanadates toxicity

Abstract

Vanadium compounds are able to interact with living cells exerting a variety of biological effects. The pentavalent form is the most stable and toxic form of the element. In systems in vitro pentavalent vanadium is an effective genotoxic agent, inducing DNA damage and chromosome malsegregation at low doses. On the other hand, no adequate in vivo data are available for the characterization of the genotoxic hazard following oral intake, the most relevant route of human exposure. In this study, the genotoxic effects produced by the oral intake of sodium ortho-vanadate (Na(3)VO(4)) were investigated. Male CD-1 mice were treated for 5 weeks with a range of concentrations of Na(3)VO(4) in drinking water (0.75-1500 mg/l). Both micronuclei and primary DNA lesions as detected by comet assay were assessed in several tissues. Statistically significant increases of micronuclei in bone marrow were observed in mice receiving the two highest concentrations of Na(3)VO(4) (750 and 1500 mg/l). A significant increase of comet tail length was observed in splenocytes of mice receiving Na(3)VO(4) at 1500 mg/l, whereas no effect was observed in bone marrow and testis cells. No treatment-related effect on sperm chromatin structure or on testis cell population was observed. The determination of vanadium content in mouse tissues at the end of treatment highlighted a very low internal exposure, especially in soft tissues. Overall, the results obtained indicate that the genotoxic activity of pentavalent vanadium is expressed in vivo only following high dose exposure, possibly as a consequence of the poor bioavailability of the element.

Published

2005

13. Exposure to PCBs and p,p'-DDE and human sperm chromatin integrity.

Author

Rignell-Hydbom A, Rylander L, Giwercman A, Jönsson BA, Lindh C, Eleuteri P, Rescia M, Leter G, Cordelli E, Spano M, and Hagmar L

Subjects

Adult, Aged, Chromatin drug effects, Dichlorodiphenyl Dichloroethylene blood, Environmental Monitoring, Environmental Pollutants blood, Flow Cytometry, Humans, Lipids analysis, Male, Middle Aged, Polychlorinated Biphenyls blood, Sweden, DNA Damage, Dichlorodiphenyl Dichloroethylene toxicity, Environmental Pollutants toxicity, Polychlorinated Biphenyls toxicity, Spermatozoa drug effects

Abstract

Persistent organochlorine pollutants (POPs) such as polychlorinated biphenyls (PCBs) and dichlorodiphenyldichloroethylene (p,p'-DDE), the major metabolite of dichlorodiphenyltrichloroethane (DDT), are stable lipophilic compounds widely found in the environment and in the general population. They can enter the food chain, and their negative impact on male reproduction is currently under active scrutiny. To explore the hypothesis that environmental exposure to these compounds is associated with altered sperm chromatin structure integrity in human sperm, we conducted a study of 176 Swedish fishermen (with low and high consumption of fatty fish, a very important exposure source of POPs). We determined serum levels of 2,2',4,4',5,5'-hexachlorobiphenyl (CB-153) and p,p'-DDE, and we used the sperm chromatin structure assay (SCSA) to assess sperm DNA/chromatin integrity. When CB-153 serum levels (individual dose range, 39-1,460 ng/g lipid) were categorized into equally sized quintiles, we found an association with the DNA fragmentation index (%DFI). A significantly lower %DFI was found in the lowest CB-153 quintile (< 113 ng/g lipid) compared with the other quintiles; there was a similar tendency, although not statistically significant, between %DFI and p,p'-DDE. These results suggest that POP exposure may have a slight negative impact on human sperm chromatin integrity.

Published

2005

14. Melphalan-induced DNA damage in p53(+/-) and wild type mice analysed by the comet assay.

Author

Cordelli E, Cinelli S, Lascialfari A, Ranaldi R, and Pacchierotti F

Subjects

Animals, Antineoplastic Agents, Alkylating pharmacology, Cross-Linking Reagents pharmacology, Dose-Response Relationship, Drug, Genotype, Intestines radiation effects, Liver radiation effects, Mice, Mice, Inbred C57BL, Mice, Knockout, Mice, Transgenic, Time Factors, Tissue Distribution, X-Rays, Comet Assay methods, DNA Damage, Genes, p53, Melphalan pharmacology

Abstract

Melphalan is an alkylating substance used as a therapeutic agent; its mutagenicity is related to its ability to produce monoadducts and to form DNA cross-links. The alkaline comet assay is a useful test for the detection of DNA lesions. However, cross-links are not easily detected under standard conditions. Recently, modifications to the test have been introduced to measure cross-links by evaluating the reduction in induced DNA migration. In this work, the standard comet assay and an assay modified by prolonging the electrophoresis time have been applied to evaluate DNA lesions induced by single, 4 or 26 weekly oral administrations of melphalan to p53(+/-) knockout and to isotype parental mice. Cells were analysed from the liver, bone marrow, peripheral blood and the distal intestine. Moreover, a further protocol in which the presence of cross-links was inferred by the reduction in X-ray-induced DNA migration was applied to bone marrow cells and the sensitivity of the different methods was compared. The majority of groups examined by the standard protocol showed no difference compared to controls, while the modified protocol (prolonged electrophoresis time) could detect a retarded DNA migration in cells from all the organs analysed with the exception of bone marrow cells. Only the protocol based on X-ray in vitro irradiation showed the presence of melphalan-induced cross-links in bone marrow cells exposed to 2mg/kg for 4 weeks, demonstrating that this was the most sensitive approach for detecting this type of lesion. DNA lesions were evident in all the organs analysed. However, results suggest that the kinetics of cross-link repair could be different in bone marrow cells compared to other organs tested. After comparison between genotype-matched treated and control groups, a significant effect was shown more frequently in p53(+/-) than in wild type groups.

Published

2004

15. Evaluation of DNA damage in different stages of mouse spermatogenesis after testicular X irradiation.

Author

Cordelli E, Fresegna AM, Leter G, Eleuteri P, Spanò M, and Villani P

Subjects

Animals, Cells, Cultured, Chromatin ultrastructure, Dose-Response Relationship, Radiation, Male, Mice, Spermatozoa cytology, Testis cytology, Testis growth & development, Chromatin radiation effects, DNA Damage, Spermatogenesis radiation effects, Spermatozoa radiation effects, Testis radiation effects

Abstract

To evaluate whether DNA alterations in mature spermatozoa could stem from DNA damage induced in immature germ cells, testis cells and spermatozoa were analyzed by the comet assay and by the sperm chromatin structure assay 14, 45 and 100 days after in vivo X irradiation of the testes. These times were selected, according to the mouse seminiferous epithelium cycle, to follow the DNA damage induced in different germ cell compartments. The cytotoxic action was assessed by DNA flow cytometric analysis of testicular cells. A dose-dependent increase of DNA damage in testis cells was observed 14 days after irradiation, whereas mature sperm cells were not affected. On the other hand, an increase in DNA strand breaks was seen in spermatozoa 45 days after treatment. DNA damage returned to the control levels 100 days after irradiation. The methods used to evaluate DNA damage gave comparable results, emphasizing the correlation between DNA fragmentation and susceptibility of sperm chromatin to denaturation. Both techniques showed the high radiosensitivity of differentiating spermatogonia. The overall results showed that DNA damage induced in pre-meiotic germ cells is detectable in primary spermatocytes and is still present in mature spermatozoa.

Published

2003

16. Analysis of DNA oxidative damage related to cell proliferation.

Author

Villani P, Altavista PL, Castaldi L, Leter G, and Cordelli E

Subjects

Animals, Cell Cycle drug effects, Cell Division drug effects, Cells, Cultured, Comet Assay, DNA analysis, DNA Repair drug effects, Dose-Response Relationship, Drug, Flow Cytometry, Hydrogen Peroxide pharmacology, Mice, Micronucleus Tests, Oxidants pharmacology, Oxidation-Reduction drug effects, DNA drug effects, DNA Damage, Fibroblasts cytology, Fibroblasts drug effects

Abstract

In vivo and in vitro cell populations exhibit a different sensitivity and a heterogeneous response to many genotoxic agents. Several studies have been carried out to evaluate the possibility that the different sensitivity of the cells is related to their proliferative status. In this study, the sensitivity of proliferating (P) and quiescent (Q) C3H10T1/2 cells to oxidative damage and their repair capability has been investigated by single cell gel electrophoresis (SCGE) and micronucleus test. Furthermore the possibility to simultaneously detect DNA damage and cell cycle position has been evaluated. Our results showed a dose-related increase of DNA damage in exponential and plateau phase cells treated with hydrogen peroxide (doses ranging between 2.5 and 100 microM). DNA damage was almost completely repaired within 2 h after treatment in both culture conditions. The percentage of cells in the various phases of the cell cycle has been determined by comet assay and by flow cytometry, and a good agreement between the results of the two techniques was found. Untreated exponentially growing cells in G1 phase showed a lower tail moment than S and G2/M cells. The same cell cycle dependence was evidenced in cells treated with low doses of H(2)O(2), while, at the higher doses, all cells showed a similar level of damage. These results confirm the sensitivity of the Comet Assay in assessing DNA damage, and support its usefulness in evaluating cell cycle-related differential sensitivity to genotoxic agents.

Published

2000

17. Sperm chromatin damage impairs human fertility. The Danish First Pregnancy Planner Study Team.

Author

Spanò M, Bonde JP, Hjøllund HI, Kolstad HA, Cordelli E, and Leter G

Subjects

Female, Flow Cytometry, Humans, Male, Pregnancy, Sperm Count, Sperm Motility, Chromatin ultrastructure, DNA Damage, Infertility, Male etiology, Spermatozoa chemistry

Abstract

Objective: To examine the relationship between sperm chromatin defects, evaluated by the flow cytometric (FCM) sperm chromatin structure assay (SCSA), and the probability of a pregnancy in a menstrual cycle (fecundability)., Design: Follow-up study., Setting: The Section of Toxicology and Biomedical Sciences, ENEA Casaccia, Rome, Italy, and the Department of Occupational Medicine, Aarhus University Hospital, Aarhus, Denmark., Patient(s): Two hundred fifteen Danish first pregnancy planners with no previous knowledge of their fertility capability., Intervention(s): None., Main Outcome Measure(s): Semen samples were collected at enrollment to measure semen volume, sperm concentration, motility, and morphology (by microscopy), as well as chromatin susceptibility to in situ, acid-induced partial denaturation by the FCM SCSA. Time to pregnancy was evaluated during a 2-year follow-up period. Demographic, medical, reproductive, occupational, and lifestyle data were collected by questionnaire. Fecundability was correlated with SCSA-derived parameters., Result(s): Fecundability declines as a function of the percentage of sperm with abnormal chromatin and becomes small when aberrant cells are >40%., Conclusion(s): Optimal sperm chromatin packaging seems necessary for full expression of the male fertility potential. The SCSA emerged as a predictor of the probability to conceive in this population-based study.

Published

2000

18. DNA integrity in human sperm.

Author

Anderson D, Dobrzyńska MM, Yu TW, Gandini L, Cordelli E, and Spano M

Subjects

Flow Cytometry, Humans, Infertility, Male metabolism, Male, DNA drug effects, DNA Damage, Spermatozoa chemistry

Abstract

Since the 1970s there have been conflicting reports of decreasing sperm counts in man and increasing testicular cancer. There is a hypothetical link between apparent adverse trends in several measures of human reproductive health and exposure to endocrine disrupters. Rodent bioassays are not suited for the large-scale screening of such chemicals because of their costs, complexity, and ethical concerns. Various in vitro assays have been used to examine the effects of these chemicals, but none has directly used semen as one of the target tissues in man. The present study has examined in the alkaline Comet assay in human sperm the effect of two estrogens--beta-estradiol and the phytoestrogen daidzein--and 1,2-epoxybutene, a metabolite of 1,3-butadiene, and compared them with the effects of the known reprotoxin, dibromochloropropane, in two fertile and two infertile frozen sperm samples and two fresh fertile samples. While differences were detected in the frozen fertile and infertile samples with flow cytometry, in the Comet assay both frozen and fresh samples exposed to the chemicals in vitro from fertile and infertile men produced similar altered responses by comparison with untreated samples. The integrity of DNA is necessary not only for the noncancerous state, but also for the accurate transmission of genetic material to the next generation. Thus this assay may be useful for examination of chemicals in fresh and frozen sperm samples.

Published

1997

19. γ-H2AX detection in somatic and germ cells of mice

Author

Paris, L., Cordelli, E., Paris, L., and Cordelli, E.

Subjects

Mouse, γ-H2AX, Germ cells, DNA damage, Bone marrow, Flow cytometry, Immunocytochemistry, Germ cell

Abstract

The phosphorylation of histone H2AX at serine 139 (γ-H2AX) is one of the first steps of DNA damage response and its detection is widely used as a sensitive marker for DNA double-strand breaks induced by ionizing radiation or other genotoxic agents. Immuno-stained phosphorylated histone can be measured in single cells by flow cytometry or single γ-H2AX foci can be visualized and counted microscopically in histological or cytological preparations. Animal studies are well recognized as important tools to study mechanisms of in vivo response to genotoxic stress. Tissues are composed by many cell types differing for function, differentiation, and proliferative capacity. In particular, due to the complexity of spermatogenesis and the heterogeneity of testicular cell subpopulations, an accurate characterization of damage in this tissue is difficult and requires an approach which allows the identification of damage in the different cellular compartments. This chapter presents techniques for γ-H2AX detection in mouse bone marrow and testicular cells. Furthermore, advantages and weaknesses of flow cytometric and microscopic methods are described. © Springer Science+Business Media, New York 2013.

Published

2013

20. 935 MHz cellular phone radiation. An in vitro study of genotoxicity in human lymphocytes.

Author

Stronati, L., Testa, A., Moquet, J., Edwards, A., Cordelli, E., Villani, P., Marino, C., Fresegna, A. M., Appolloni, M., and Lloyd, D.

Subjects

LYMPHOCYTES, RADIOGRAPHY, RADIO frequency, CELL phones, DNA damage, BIOCHEMICAL genetics

Abstract

Purpose: The possibility of genotoxicity of radiofrequency radiation (RFR) applied alone or in combination with x-rays was investigated in vitro using several assays on human lymphocytes. The chosen specific absorption rate (SAR) values are near the upper limit of actual energy absorption in localized tissue when persons use some cellular telephones. The purpose of the combined exposures was to examine whether RFR might act epigenetically by reducing the fidelity of repair of DNA damage caused by a well-characterized and established mutagen. Methods: Blood specimens from 14 donors were exposed continuously for 24 h to a Global System for Mobile Communications (GSM) basic 935 MHz signal. The signal was applied at two SAR; 1 and 2 W/Kg, alone or combined with a 1-min exposure to 1.0 Gy of 250 kVp x-rays given immediately before or after the RFR. The assays employed were the alkaline comet technique to detect DNA strand breakage, metaphase analyses to detect unstable chromosomal aberrations and sister chromatid exchanges, micronuclei in cytokinesis-blocked binucleate lymphocytes and the nuclear division index to detect alterations in the speed of in vitro cell cycling. Results: By comparison with appropriate sham-exposed and control samples, no effect of RFR alone could be found for any of the assay endpoints. In addition RFR did not modify any measured effects of the x-radiation. Conclusions: This study has used several standard in vitro tests for chromosomal and DNA damage in Go human lymphocytes exposed in vitro to a combination of x-rays and RFR. It has comprehensively examined whether a 24-h continuous exposure to a 935 MHz GSM basic signal delivering SAR of 1 or 2 W/Kg is genotoxic per se or whether, it can influence the genotoxicity of the well-established clastogenic agent; x-radiation. Within the experimental parameters of the study in all instances no effect from the RFR signal was observed. [ABSTRACT FROM AUTHOR]

Published

2006

21. Sperm chromatin damage impairs human fertility. The Danish First Pregnancy Planner Study Team

Author

Spanò, M., Bonde, J. P., Niels Henrik I Hjollund, Henrik Kolstad, Cordelli, E., and Leter, G.

Subjects

Male, endocrine system, Sperm Count, urogenital system, Flow Cytometry, Spermatozoa, Chromatin, Pregnancy, Sperm Motility, Humans, Female, reproductive and urinary physiology, Infertility, Male, DNA Damage

Abstract

To examine the relationship between sperm chromatin defects, evaluated by the flow cytometric (FCM) sperm chromatin structure assay (SCSA), and the probability of a pregnancy in a menstrual cycle (fecundability).

22. Clinical and genomic safety of treatment with Ginkgo biloba L. leaf extract (IDN 5933/Ginkgoselect®Plus) in elderly: A randomised placebo-controlled clinical trial [GiBiEx]

Author

Stefano Bonassi, Vanessa Valdiglesias, Francesca Pacchierotti, Giuseppe Rasoni, Palma Lamonaca, Eugenia Cordelli, Marzia Ruggi, Martina Panatta, Raffaella Rossi, María Sánchez-Flores, Giulia Prinzi, Barbara Benassi, Salvatore Malandrino, Patrizia Russo, Irene Paximadas, Paola Villani, Cordelli, E., Panatta, M., Villani, P., Pacchierotti, F., and Benassi, B.

Subjects

0301 basic medicine, Male, Genomic stability, medicine.medical_specialty, Population, Placebo, Gastroenterology, law.invention, 03 medical and health sciences, Randomized controlled trial, Liver Function Tests, law, Internal medicine, Medicine, Humans, DNA cell maintenance, education, Aged, Liver injury, Aged, 80 and over, education.field_of_study, Genome, Micronucleus Tests, biology, business.industry, Ginkgo biloba, Plant Extracts, Incidence (epidemiology), General Medicine, lcsh:Other systems of medicine, Ginkgo biloba Extract, Safety, biology.organism_classification, medicine.disease, lcsh:RZ201-999, Clinical trial, Plant Leaves, 030104 developmental biology, Complementary and alternative medicine, Liver, Micronucleus test, Female, business, Research Article, DNA Damage

Abstract

Background Numerous health benefits have been attributed to the Ginkgo biloba leaf extract (GBLE), one of the most extensively used phytopharmaceutical drugs worldwide. Recently, concerns of the safety of the extract have been raised after a report from US National Toxicology Program (NTP) claimed high doses of GBLE increased liver and thyroid cancer incidence in mice and rats. A safety study has been designed to assess, in a population of elderly residents in nursing homes, clinical and genomic risks associated to GBLE treatment. Methods GiBiEx is a multicentre randomized clinical trial, placebo controlled, double blinded, which compared subjects randomized to twice-daily doses of either 120-mg of IDN 5933 (also known as Ginkgoselect®Plus) or to placebo for a 6-months period. IDN 5933 is extracted from dried leaves and contains 24.3% flavone glycosides and 6.1% of terpene lactones (2.9% bilobalide, 1.38% ginkgolide A, 0.66% ginkgolide B, 1.12% ginkgolide C) as determined by HPLC. The study was completed by 47 subjects, 20 in the placebo group and 27 in the treatment group. Clinical (adverse clinical effect and liver injury) and genomic (micronucleus frequency, comet assay, c-myc, p53, and ctnnb1 expression profile in lymphocytes) endpoints were assessed at the start and at the end of the study. Results No adverse clinical effects or increase of liver injury markers were reported in the treatment group. The frequency of micronuclei [Mean Ratio (MR) = 1.01, 95% Confidence Intervals (95% CI) 0.86–1.18), and DNA breaks (comet assay) (MR = 0.91; 95% CI 0.58–1.43), did not differ in the two study groups. No significant difference was found in the expression profile of the three genes investigated. Conclusions None of the markers investigated revealed a higher risk in the treatment group, supporting the safety of IDN 5933 at doses prescribed and for duration of six months. Trial registration ClinicalTrials.gov Identifier: NCT03004508, December 20, 2016. Trial retrospectively registered. Electronic supplementary material The online version of this article (10.1186/s12906-018-2080-5) contains supplementary material, which is available to authorized users.

Published

2018

23. Study of TiO2 P25 Nanoparticles Genotoxicity on Lung, Blood, and Liver Cells in Lung Overload and Non-Overload Conditions After Repeated Respiratory Exposure in Rats

Author

Patrizia Eleuteri, Charlène Relier, Jorge Mejia, Bénédicte Trouiller, Franck Robidel, Ghislaine Lacroix, Marielle Dubreuil, Stéphane Lucas, Thomas Loret, Eugenia Cordelli, Francesca Pacchierotti, Omar Lozano Garcia, Institut National de l'Environnement Industriel et des Risques (INERIS), Italian National Agency for New Technologies, Energy and Sustainable Economic Development (ENEA), Périnatalité et Risques Toxiques - UMR INERIS_I 1 (PERITOX), Université de Picardie Jules Verne (UPJV)-CHU Amiens-Picardie-Institut National de l'Environnement Industriel et des Risques, Pacchierotti, F., Eleuteri, P., and Cordelli, E.

Subjects

0301 basic medicine, Male, Pathology, medicine.medical_specialty, Erythrocytes, Cell Survival, Surface Properties, TITANIUM DIOXIDE, Inflammation, Pharmacology, Gene mutation, Toxicology, medicine.disease_cause, Rodents, Nanomaterials, DNA damage, Titanium dioxide, Glutathione, Rats, Sprague-Dawley, 03 medical and health sciences, INFLAMMATION, medicine, GLUTATHIONE, RODENTS, Animals, Tissue Distribution, Respiratory system, Particle Size, Lung, NANOMATERIALS, Titanium, Inhalation Exposure, Rodent, Dose-Response Relationship, Drug, business.industry, 030111 toxicology, respiratory system, Nanomaterial, 3. Good health, Oxidative Stress, medicine.anatomical_structure, Liver, [SDV.TOX]Life Sciences [q-bio]/Toxicology, Toxicity, Nanoparticles, medicine.symptom, business, Genotoxicity, Oxidative stress, Respiratory tract, DNA Damage, Mutagens

Abstract

Inhaled titanium dioxide (TiO 2) nanoparticles (NPs) can have negative health effects, and have been shown to cause respiratory tract cancer in rats. Inflammation has been linked to oxidative stress, and both have been described as possible mechanisms for genotoxicity of NPs, but rarely examined side-by-side in animal studies. In the present study, a wide range of complementary endpoints have been performed to study TiO 2 P25NP-induced genotoxicity in lung overload and non-overload conditions. Additionally, lung burden, inflammation, cytotoxicity and oxidative stress have also been evaluated in order to link genotoxicity with these responses. To assess quick and delayed responses after recovery, endpoints were evaluated at two time points: 2 h and 35 days after three repeated instillations. This study confirmed the previously described lung overload threshold at approximately 200-300cm 2 of lung burden for total particle surface area lung deposition or 4.2 ml/kg for volume-based cumulative lung exposure dose, above which lung clearance is impaired and inflammation is induced. Our results went on to show that these overload doses induced delayed genotoxicity in lung, associated with persistent inflammation only at the highest dose. The lowest tested doses had no toxicity or genotoxicity effects in the lung. In blood, no lymphocyte DNA damage, erythrocytes chromosomal damage or gene mutation could be detected. Our data also demonstrated that only overload doses induced liver DNA lesions irrespective of the recovery time. Tested doses of TiO 2 P25 NPs did not induce glutathione changes in lung, blood or liver at both recovery times.

Published

2017

24. Cytotoxicity, genotoxicity and gene expression changes elicited by exposure of human hepatic cells to Ginkgo biloba leaf extract

Author

Irene Paximadas, Maria Giuseppa Grollino, Salvatore Malandrino, Giuseppe Raschellà, Stefano Bonassi, Marco Pieraccioli, Paola Villani, Francesca Pacchierotti, Eugenia Cordelli, Pacchierotti, F., Villani, P., Cordelli, E., Raschellà, G., and Grollino, M. G.

Subjects

0301 basic medicine, HepG2, Cell Survival, Cytotoxicity, Gene Expression, Pharmacology, Toxicology, medicine.disease_cause, Cell Line, 03 medical and health sciences, 0302 clinical medicine, THLE-2, medicine, Humans, Viability assay, Carcinogen, chemistry.chemical_classification, Reactive oxygen species, biology, Ginkgo biloba, Plant Extracts, Ginkgo, Molecular analysis, General Medicine, biology.organism_classification, Comet assay, Plant Leaves, 030104 developmental biology, Insulin-Like Growth Factor Binding Protein 3, chemistry, Apoptosis, Genotoxicity, 030220 oncology & carcinogenesis, Hepatocytes, Comet Assay, Reactive Oxygen Species, Food Science, DNA Damage

Abstract

The use of Ginkgo biloba leaf extract as nutraceutical is becoming increasingly common. As a consequence, the definition of a reliable toxicological profile is a priority for its safe utilization. Recently, contrasting data have been reported on the carcinogenic potential of Ginkgo biloba extract in rodent liver. We measured viability, Reactive Oxygen Species (ROS), apoptosis, colony-forming efficiency, genotoxicity by comet assay, and gene expression changes associated with hepato-carcinogenicity in human cells of hepatic origin (HepG2 and THLE-2) treated with different concentrations (0.0005–1.2 mg/mL) of Ginkgoselect®Plus. Our analyses highlighted a decrease of cell viability, not due to apoptosis, after treatment with high doses of the extract, which was likely due to ROS generation by a chemical reaction between extract polyphenols and some components of the culture medium. Comet assay did not detect genotoxic effect at any extract concentration. Finally, the array analysis detected a slight decrease in the expression of only one gene (IGFBP3) in Ginkgo-treated THLE-2 cells as opposed to changes in 28 genes in Aflatoxin B1 treated-cells. In conclusion, our results did not detect any significant genotoxic or biologically relevant cytotoxic effects and gross changes in gene expression using the Ginkgo extract in the hepatic cells tested. © 2017 The Authors

Published

2017

25. X-Ray Induced DNA Damage and Repair in Germ Cells of PARP1−/− Male Mice

Author

Patrizia Eleuteri, Roberto Ranaldi, Anna Maria Fresegna, Paola Villani, Eugenia Cordelli, Lorena Paris, Francesca Pacchierotti, Cordelli, E., Pacchierotti, F., Paris, L., Eleuteri, P., Ranaldi, R., Fresegna, A. M., and Villani, P.

Subjects

Male, DNA Repair, DNA damage, DNA repair, Poly ADP ribose polymerase, Poly (ADP-Ribose) Polymerase-1, Catalysis, Chromatin remodeling, Male mouse germ cell, Article, Comet assay, H2AX phosphorylation, Ionizing radiation, Male mouse germ cells, Poly(ADP-ribose)polymerase-1, lcsh:Chemistry, Inorganic Chemistry, male mouse germ cells, Histones, Mice, PARP1, comet assay, Animals, Physical and Theoretical Chemistry, Phosphorylation, lcsh:QH301-705.5, Molecular Biology, Spectroscopy, Mice, Knockout, biology, X-Rays, Organic Chemistry, General Medicine, Flow Cytometry, Molecular biology, Computer Science Applications, Chromatin, Mice, Inbred C57BL, Histone, Germ Cells, lcsh:Biology (General), lcsh:QD1-999, biology.protein, poly(ADP-ribose)polymerase-1, Poly(ADP-ribose) Polymerases, ionizing radiation, DNA Damage

Abstract

Poly(ADP-ribose)polymerase-1 (PARP1) is a nuclear protein implicated in DNA repair, recombination, replication, and chromatin remodeling. The aim of this study was to evaluate possible differences between PARP1-/- and wild-type mice regarding induction and repair of DNA lesions in irradiated male germ cells. Comet assay was applied to detect DNA damage in testicular cells immediately, and two hours after 4 Gy X-ray irradiation. A similar level of spontaneous and radiation-induced DNA damage was observed in PARP1-/- and wild-type mice. Conversely, two hours after irradiation, a significant level of residual damage was observed in PARP1-/- cells only. This finding was particularly evident in round spermatids. To evaluate if PARP1 had also a role in the dynamics of H2AX phosphorylation in round spermatids, in which γ-H2AX foci had been shown to persist after completion of DNA repair, we carried out a parallel analysis of γ-H2AX foci at 0.5, 2, and 48 h after irradiation in wild-type and PARP1-/- mice. No evidence was obtained of an effect of PARP1 depletion on H2AX phosphorylation induction and removal. Our results suggest that, in round spermatids, under the tested experimental conditions, PARP1 has a role in radiation-induced DNA damage repair rather than in long-term chromatin modifications signaled by phosphorylated H2AX. © 2013 by the authors; licensee MDPI, Basel, Switzerland.

Published

2013

26. Genotoxicity Induced by Foetal and Infant Exposure to Magnetic Fields and Modulation of Ionising Radiation Effects

Author

Livio Giuliani, Eugenia Cordelli, Paola Villani, Francesca Pacchierotti, Caterina Tanzarella, Patrizia Eleuteri, Antonella Sgura, Ion Udroiu, Antonio Antoccia, Udroiu, Ion, Antoccia, Antonio, Tanzarella, Caterina, Giuliani, Livio, Pacchierotti, Francesca, Cordelli, Eugenia, Eleuteri, Patrizia, Villani, Paola, Sgura, Antonella, Villani, P., Eleuteri, P., Cordelli, E., and Pacchierotti, F.

Subjects

Somatic cell, Embryonic Development, lcsh:Medicine, Biology, medicine.disease_cause, Ionizing radiation, Andrology, Mice, Pregnancy, Radiation, Ionizing, medicine, Animals, lcsh:Science, Cell Proliferation, Multidisciplinary, lcsh:R, Infant exposure, Cell Differentiation, respiratory system, Teratology, Comet assay, Germ Cells, Magnetic Fields, Prenatal Exposure Delayed Effects, Toxicity, Micronucleus test, Immunology, Female, lcsh:Q, Genotoxicity, DNA Damage, Research Article

Abstract

Background: Few studies have investigated the toxicity and genotoxicity of extremely low frequency magnetic fields (ELF-MF) during prenatal and neonatal development. These phases of life are characterized by cell proliferation and differentiation, which might make them sensitive to environmental stressors. Although in vitro evidences suggest that ELF-MF may modify the effects of ionizing radiation, no research has been conducted so far in vivo on the genotoxic effects of ELF-MF combined with X-rays. Aim and methods: Aim of this study was to investigate in somatic and germ cells the effects of chronic ELF-MF exposure from mid gestation until weaning, and any possible modulation produced by ELFMF exposure on ionizing radiation-induced damage. Mice were exposed to 50 Hz, 65 μT magnetic field, 24 hours/day, for a total of 30 days, starting from 12 days post-conception. Another group was irradiated with 1 Gy X-rays immediately before ELF-MF exposure, other groups were only X-irradiated or sham-exposed. Micronucleus test on blood erythrocytes was performed at multiple times from 1 to 140 days after birth. Additionally, 42 days after birth, genotoxic and cytotoxic effects on male germ cells were assessed by comet assay and flow cytometric analysis. Results: ELF-MF exposure had no teratogenic effect and did not affect survival, growth and development. The micronucleus test indicated that ELF-MF induced a slight genotoxic damage only after the maximum exposure time and that this effect faded away in the months following the end of exposure. ELF-MF had no effects on ionizing radiation (IR)-induced genotoxicity in erythrocytes. Differently, ELF-MF appeared to modulate the response of male germ cells to X-rays with an impact on proliferation/differentiation processes. These results point to the importance of tissue specificity and development on the impact of ELF-MF on the early stages of life and indicate the need of further research on the molecular mechanisms underlying ELF-MF biological effects. © 2015 Udroiu et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Published

2015