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Dive into the research topics where Alessandra Affatato is active.

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Featured researches published by Alessandra Affatato.


Mutation Research | 2003

Induction and suppression of cytochrome P450 isoenzymes and generation of oxygen radicals by procymidone in liver, kidney and lung of CD1 mice

Andrea Sapone; Alessandra Affatato; Donatella Canistro; Massimiliano Broccoli; Silvia Trespidi; Laura Pozzetti; Gian Luigi Biagi; Giorgio Cantelli-Forti; Moreno Paolini

Although chronic administration of procymidone (a widely used dicarboximide fungicide) leads to an increased incidence of liver tumors in mice, short-term genotoxicity studies proved negative. As cytochrome P450 (CYP) induction has been linked to non-genotoxic carcinogenesis, we investigated whether procymidone administration causes induction of CYP-dependent monooxygenases in liver, kidney and lung microsomes of male Swiss Albino CD1 mice after single or repeated (daily for three consecutive days) i.p. treatment with either 400 or 800 (1/10 or 1/20 of the DL(50)) mgkg(-1) b.w. procymidone. CYP content and CYP3A1/2, 1A1, 1A2, 2B1/2, 2E1, 2A, 2D9 and 2C11 supported oxidations were studied using either the regio- and stereo-selective hydroxylation of testosterone as multibiomarker or highly specific substrates as probes of various CYPs. While a single dose was uneffective, multiple procymidone administration lead to marked inductions of various monooxygenases: CYP3A1/2 in liver and lung (as measured by N-demethylation of aminopyrine and testosterone 6 beta-hydroxylase); CYP2E1 in liver (p-nitrophenol hydroxylation); CYP1A1 in liver and kidney (deethylation of ethoxyresorufin). Several hydroxylations were induced in the liver, including the CYP2A-linked 7 alpha (14-fold) as well as 6 alpha (22-fold), 6 beta, 16 beta and 2 beta hydroxylases. The pattern of inductions/suppressions recorded in the three different tissues suggests that procymidone exerts complex effects on the CYP profile. Tissue-specific trends included a large number of inductions in the liver and suppressions in the lung. The main inductions were corroborated by immunoblotting analyses and Northern blotting showed that inductions of CYP3A1/2, CYP2E1 and CYP1A1/2 were paralleled by increased mRNA levels. It was also found that CYP over-expression generates large amounts of reactive oxygen species (ROS), especially in liver. These data may explain why in vitro short-term genotoxicity studies on procymidone were negative, whereas in vivo long-term carcinogenesis studies turned out positive: long-term CYP induction (e.g. oxygen centered free radicals over-production) can have a co-carcinogenic and/or promoting potential.


Journal of the Neurological Sciences | 2010

The novel radical scavenger IAC is effective in preventing and protecting against post-ischemic brain damage in Mongolian gerbils

Donatella Canistro; Alessandra Affatato; Antonio Soleti; Vincenzo Mollace; Carolina Muscoli; Francesca Sculco; Iolanda Sacco; Valeria Visalli; Barbara Bonamassa; Manuela Martano; Michelangelo Iannone; Andrea Sapone; Moreno Paolini

The removal of pathologically generated free radicals produced during ischemia, reperfusion and intracranical hemorrhage seems to be a viable approach to neuroprotection. However, at present, no neuroprotective agent has proven effective in focal ischemic stroke phase III trials, despite the encouraging data in animal models. This study aimed to explore the effect of the brain penetrant low molecular weight radical scavenger bis(1-hydroxy-2,2,6,6-tetramethyl-4-piperidinyl)-decandioate (IAC) in neurological damage subsequent to ischemia-reperfusion injury in Mongolian gerbils. We examined the intraperitoneal effects of IAC on temporary bilateral common carotid artery occlusion (BCCO) by means of morphological and histological analysis of the hippocampus. Significant dose-dependent protective effects of IAC (1 to 10mg/kg b.w.) against neuropathological and morphological brain changes were seen when administered i.p. 1h before temporary BCCO in Mongolian gerbils. When administered up to 6h after BCCO, IAC actually reverses the neurodegenerative processes (e.g. hippocampal cell viability) induced by ischemia in a dose-dependent fashion. Data show that IAC is highly effective in protecting and preventing oxidative brain damage associated with cerebral flow disturbances. It is also effective even in late treatment of the insult, emphasizing its potential role for the management of ischemic stroke patients.


Cancer Letters | 2002

In vitro induction of benzo(a)pyrene cell-transforming activity by the glucosinolate gluconasturtiin found in cruciferous vegetables

Paolo Perocco; Renato Iori; Jessica Barillari; Massimiliano Broccoli; Andrea Sapone; Alessandra Affatato; Moreno Paolini

Cytotoxic and cell-transforming activity of gluconasturtiin (GNST), a promising chemopreventive agent commonly found in human diet, was studied in a medium-term bioassay utilizing BALB/c 3T3 cells. We also assessed whether GNST coupled with myrosinase, thus yielding product phenylethyl isothiocyanate (as shown by gas chromatography-mass spectral analysis), can affect the transforming potential of benzo(a)pyrene (B(a)P). Neither cytotoxicity nor cell-transforming activity was recorded. On the contrary, a marked increase (up to sevenfold) of the transforming activity of B(a)P was seen. This cocarcinogenic potential could be ascribed to an imbalance among bioactivation/detoxication during cell growth. These results indicate the need for an overall toxicological characterization of a chemopreventive agent prior to large-scale use.


Mutation Research | 2006

Glucoraphanin, the bioprecursor of the widely extolled chemopreventive agent sulforaphane found in broccoli, induces Phase-I xenobiotic metabolizing enzymes and increases free radical generation in rat liver

Paolo Perocco; G. Bronzetti; Donatella Canistro; Luca Valgimigli; Andrea Sapone; Alessandra Affatato; Gian Franco Pedulli; Laura Pozzetti; Massimiliano Broccoli; Renato Iori; Jessica Barillari; Valeriana Sblendorio; Marvin S. Legator; Moreno Paolini; Sherif Z. Abdel-Rahman


Environmental and Molecular Mutagenesis | 2004

Effect of XPD/ERCC2 polymorphisms on chromosome aberration frequencies in smokers and on sensitivity to the mutagenic tobacco-specific nitrosamine NNK

Alessandra Affatato; Kevin J. Wolfe; Mirtha S. Lopez; Csilla K. Hallberg; Marinel M. Ammenheuser; Sherif Z. Abdel-Rahman


Mutation Research-genetic Toxicology and Environmental Mutagenesis | 2007

Perturbation of cytochrome P450, generation of oxidative stress and induction of DNA damage in Cyprinus carpio exposed in situ to potable surface water

Andrea Sapone; Bianca Gustavino; Monica Monfrinotti; Donatella Canistro; Massimiliano Broccoli; Laura Pozzetti; Alessandra Affatato; Luca Valgimigli; Giorgio Cantelli Forti; Gian Franco Pedulli; Gian Luigi Biagi; Sherif Z. Abdel-Rahman; Moreno Paolini


Environmental and Molecular Mutagenesis | 2005

Gender differences in genetic damage induced by the tobacco-specific nitrosamine NNK and the influence of the Thr241Met polymorphism in the XRCC3 gene.

Courtney E. Hill; Alessandra Affatato; Kevin J. Wolfe; Mirtha S. Lopez; Csilla K. Hallberg; Donatella Canistro; Sherif Z. Abdel-Rahman


Food and Chemical Toxicology | 2005

CYP superfamily perturbation by diflubenzuron or acephate in different tissues of CD1 mice.

Andrea Sapone; Laura Pozzetti; Donatella Canistro; Massimiliano Broccoli; G. Bronzetti; G. Potenza; Alessandra Affatato; Gian Luigi Biagi; Giorgio Cantelli-Forti; Moreno Paolini


Mutation Research-reviews in Mutation Research | 2007

Cruciferous vegetables and lung cancer.

Andrea Sapone; Alessandra Affatato; Donatella Canistro; Laura Pozzetti; Massimiliano Broccoli; Jessica Barillari; Renato Iori; Moreno Paolini


Food and Chemical Toxicology | 2008

Perturbation of murine liver cyp-superfamily of isoforms by different combinations of pesticide mixtures.

Donatella Canistro; Laura Pozzetti; Andrea Sapone; Massimiliano Broccoli; Alessandra Affatato; A. Stradiotti; V. Longo; P. Menichini; R. Barale; Moreno Paolini

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Sherif Z. Abdel-Rahman

University of Texas Medical Branch

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Kevin J. Wolfe

University of Texas Medical Branch

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