139 results on '"Vivarelli, F."'
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2. Aspetti tossicologici legati all'utilizzo dei nuovi dispositivi elettronici per il rilascio di nicotina
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Canistro D, Vivarelli F, Cirillo S, Buschini A, Lazzaretti M, Cardenia V, Rodriguez Estrada M, Franchi P, Lucarini M, Lodovici M, Lorenzini A, Marchionni S, Croco E, Turrini E, Fimognari C, Burattini S, Falcieri E, Paolini M., and Canistro D, Vivarelli F, Cirillo S, Buschini A, Lazzaretti M, Cardenia V, Rodriguez Estrada M, Franchi P, Lucarini M, Lodovici M, Lorenzini A, Marchionni S, Croco E, Turrini E, Fimognari C, Burattini S, Falcieri E, Paolini M.
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Danno polmonare ,Stress ossidativo ,Sigaretta elettronica - Abstract
L’Organizzazione Mondiale della Sanità (OMS) ha recentemente stigmatizzato l’abitudine al fumo come una delle più gravi emergenze sanitarie globali. I dispositivi elettronici per il rilascio di nicotina (DERN), o sigarette elettroniche (e-cigs) sono state immesse sul mercato proprio con lo scopo di fornire al soggetto fumatore la possibilità di assumere nicotina esalando vapore, da un sistema che non prevede la combustione, e proposti al pubblico come metodi a “ridotto rischio per la salute”. Largamente diffusi, specialmente tra i più giovani, in alcuni paesi sono stati addirittura inclusi nei programmi integrati di lotta al tabagismo. Tuttavia, ad oggi, alcuni prestigiosi enti scientifici come il National Institute for Health and Care Excellence (NICE) ha ribadito come i dati sui possibili effetti tossicologici siano ancora limitati esortando la comunità scientifica a condurre studi indipendenti. Negli ultimi anni il nostro gruppo di ricerca ha studiato alcuni aspetti tossicologici associati all’esposizione dei vapori di e-cigs nel modello animale. Abbiamo rilevato aldeidi tossiche nello svapato e nei polmoni di ratto esposto per 4 settimane ed è stato osservato un marcato incremento degli enzimi del metabolismo degli xenobiotici, elevate concentrazione di radicali liberi (ROS), e una inattivazione dei principali enzimi antiossidanti in linea con i marcatori di danno ossidativo a livello sistemico e d’organo (DNA, lipidi, proteine). Test di mutagenesi effettuati su sangue e urine (comet, micronulcei, Ames) hanno evidenziato la potenzialità genotossica associata all’esposizione di e-cig. E’ interessante notare come i risultati delle analisi emocitometriche mostrino l’andamento tipico di pazienti affetti da brocopneumopatie ostruttive (COPD), con un marcato aumento dei neutrofili. I nostri studi hanno inoltre dimostrato come la scelta dell’atomizzatore, quindi del valore di resistenza applicata al sistema, sia inversamente associato alle concentrazioni di ROS e composti carbonilici rilasciati come formaldeide, acetaldeide e acroleina, indipendentemente dal voltaggio applicato. I dati in vivo confermano l’ipotesi di una tossicità direttamente dipendente dal tipo di atomizzatore scelto dal consumatore a parità di condizioni sperimentali. I risultati evidenziano inoltre come resistenze sub-Ohmiche producano un danno più marcato all’epitelio tracheale, mentre a livello polmonare, le immagini di microscopia elettronica mostrano come passando da un atomizzatore a resistenza di 1,5 Ohm a valori sub-Ohmici, il conseguente aumento del vattaggio determini una riduzione del numero e diametro dei bronchioli, fino ad una marcata disorganizzazione del parenchima polmonare con collasso alveolare, presenza di cellule in apoptosi e necrosi. Nel complesso, i risultati suggeriscono come l’utilizzo di e-cig possa costituire un serio rischio per la salute e che la personalizzazione del dispositivo e le modalità di utilizzo influenzino significativamente il rilascio di composti tossici e l’impatto sul sistema respiratorio.
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- 2020
3. Effetti co-cancerogeni della vitamina E a livello prostatico
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Vivarelli F, Canistro D, Cirillo S, Papi A, Spisni E, Vornoli A, Della Croce MC, Franchi P, Lucarini M, Zanzi C, Rotondo F, Lorenzini A, Marchionni S, Paolini M., and Vivarelli F, Canistro D, Cirillo S, Papi A, Spisni E, Vornoli A, Della Croce MC, Franchi P, Lucarini M, Zanzi C, Rotondo F, Lorenzini A, Marchionni S, Paolini M.
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Prostata ,co.cancerogenesi ,Vitamina E - Abstract
Numerosi studi sperimentali suggeriscono un ruolo chemiopreventivo della vitamina E (VE) nei confronti di numerose patologie tumorali incluso il cancro alla prostata (CA). Tuttavia, le evidenze epidemiologiche più recenti non confermano tale ipotesi, e lo studio clinico SELECT ha addirittura evidenziato un aumento dell’incidenza di CA alla prostata in pazienti sani al momento dell’arruolamento, ai quali era stata somministrata VE giornalmente alla dose di 400 UI/die. Essendo noto in letteratura come alcune isoforme del citocromo P450 (CYP) siano sovra espresse in lesioni prostatiche maligne, e che la VE, agisca come induttore del CYP in alcuni tessuti, abbiamo ipotizzato che l’aumento dell’incidenza di CA possa coinvolgere un meccanismo co-cancerogenico legato all’induzione CYP. L’esposizione a VE produce una marcata induzione del CYP in cellule epiteliali di prostata RWPE-1, incluse le isoforme responsabili dell’attivazione degli Idrocarburi Policiclici Aromatici (IPA), accompagnata da un significativo aumento delle specie reattive dell’ossigeno (ROS). Inoltre, il pathway pro-infiammatorio COX-2-dipendente risulta incrementato, caratteristica che si osserva in diverse forme tumorali incluso quelle che interessano la prostata. Il fenomeno è stato confermato nel modello animale; è stato osservato un aumento delle monoossigenasi e dell’espressione genica di alcune isoforme CYP a livello prostatico unito a una maggiore concentrazione di ROS, in linea con marcatori di danno ossidativo a livello proteico e lipidico, nella prostata di ratto. L’esposizione di cellule IMR90 a VE ha evidenziato un effetto genotossico riportando un’aumentata frequenza dei micronuclei (MN). Il potenziale co-cancerogeno di VE è stato poi confermato dallo studio della trasformazione cellulare mediate l’uso di cellule BALB/c 3T3. Cellule pre-incubate con VE e successivamente esposte a benzo[a]pirene mostrano un significativo incremento della frequenza di trasformazione rispetto a quello senza della vitamina. Il presente studio dimostra come la VE possa, in determinate condizioni, agire come co-cancerogeno tramite un meccanismo CYP-dipendente, causando danno al DNA e promovendo la trasformazione cellulare.
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- 2020
4. The pharmacological basis of the curcumin nutraceutical uses: an update
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Canistro, D., primary, Chiavaroli, A., additional, Cicia, D., additional, Cimino, F., additional, Curro, D., additional, Dell Agli, M., additional, Ferrante, C., additional, Giovannelli, L., additional, Leone, S., additional, Martinelli, G., additional, Milella, L., additional, Pagano, E., additional, Piazza, S., additional, Ponticelli, M., additional, Recinella, L., additional, Ristori, S., additional, Sangiovanni, E., additional, Smeriglio, A., additional, Speciale, A., additional, Trombetta, D., additional, and Vivarelli, F., additional
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- 2021
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5. Genotossicità della vitamina E e disregolazione dell’omeostasi redox e del metabolismo degli xenobiotici
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VIVARELLI F., M. PAOLINI, S. CIRILLO, S. MARCHIONNI, A. LORENZINI, D. CANISTRO, and VIVARELLI F., M. PAOLINI, S. CIRILLO, S. MARCHIONNI, A. LORENZINI, D. CANISTRO
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Vitamina E, equilibrio redox, genotossicità - Published
- 2018
6. Digestibility, toxicity and metabolic effects of rapeseed and sunflower protein hydrolysates in mice
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Canistro, D, Vivarelli, F, Ugolini, L, Pinna, C, Grandi, M, Antonazzo, I, Cirillo, S, Sapone, A, Cinti, S, Lazzeri, L, Conte, E, Biagi, G, Canistro D., Vivarelli F., Ugolini L., Pinna C., Grandi M., Antonazzo I. C., Cirillo S., Sapone A., Cinti S., Lazzeri L., Conte E., Biagi G., Canistro, D, Vivarelli, F, Ugolini, L, Pinna, C, Grandi, M, Antonazzo, I, Cirillo, S, Sapone, A, Cinti, S, Lazzeri, L, Conte, E, Biagi, G, Canistro D., Vivarelli F., Ugolini L., Pinna C., Grandi M., Antonazzo I. C., Cirillo S., Sapone A., Cinti S., Lazzeri L., Conte E., and Biagi G.
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The digestibility (in vitro), toxicity and metabolic effects of rapeseed (RPH) and sunflower (SPH) protein hydrolysates have been evaluated in a murine animal model. The enzyme Alcalase® was employed to obtain a mild enzymatic hydrolysis of rapeseed and sunflower defatted seed meals (DSM) protein isolates. Both hydrolysates showed higher in vitro digestibility than the respective DSM, presumably as a consequence of the hydrolysis process that they had undergone. In vivo, RPH and SPH were well tolerated. Body and organ weights, biochemical blood parameters from treated male mice were comparable to controls. Food intake was regular in RPH and SPH animals, suggesting a good palatability of the hydrolysates. Not relevant perturbations of the principal hepatic and renal drug metabolism enzymes were observed in RPH or SPH mice. In conclusion, protein hydrolysates from sunflower and rapeseed DSM did not determine relevant toxicological effects; therefore, they could be considered as alternative protein sources and/or food ingredients.
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- 2017
7. The prediction of protein secondary structure with a Cascade Correlation Learning Architecture of neural networks
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Vivarelli, F., Fariselli, P., and Casadio, R.
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- 1997
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8. E-cigarettes induce toxicological effects that can raise the cancer risk. The contribute of EPR radical trapping technique
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CANISTRO D., VIVARELLI F., CIRILLO S., BABOT MARQUILLAS C., SAPONE A., PAOLINI M, FRANCHI P, LUCARINI M., Canistro, D., Vivarelli, F., Cirillo, S., BABOT MARQUILLAS, C., Sapone, A., Paolini, M, Franchi, P, and Lucarini, M.
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E-cigarette, EPR radical probe technique, toxicology, rat - Abstract
E-cigarettes induce toxicological effects that can raise the cancer risk. The contribute of EPR radical probe technique Donatella Canistro1, Fabio Vivarelli1, Silvia Cirillo1, Andrea Sapone1, Moreno Paolini1, Paola Franchi2, Marco Lucarini2 1Department of Pharmacy and Biotechnology (University of Bologna, Via Irnerio 48, I-40126 Bologna, Italy) 2Department of Chemistry “G. Ciamician” (University of Bologna, Via San Giacomo 11, I-40126 Bologna, Italy) E-mail: paola.franchi@unibo.it Electronic cigarettes (e-cigs) are devices designed to deliver nicotine in a vaping solution rather than smoke and without tobacco combustion. Perceived as a safer alternative to conventional cigarettes, e-cigs are aggressively marketed as lifestyle-choice consumables, thanks to few restrictions and a lack of regulatory guidelines. Despite the burgeoning worldwide consumption of e-cigs, their safety remains largely unproven and it is unknown whether these devices cause in vivo toxicological effects that could contribute to cancer. Here we illustrate the contribute of EPR radical probe technique in a study where it was possible to demonstrate the co-mutagenic and cancer-initiating effects of e-cig vapour in a rat lung model. It was found that e-cig have a powerful booster effect on phase-I carcinogen-bioactivating enzymes, and increase oxygen free radical production and DNA oxidation. We are able to indirectly evaluate the content of reactive oxygen species (ROS) in lungs tissues of exposed rats, by using an appropriate hydroxylamine that in the presence of transient radical species gives rise to a persistent nitroxide radical. (see Scheme 1) Scheme 1 We found a significant increase of radical species production in samples of lungs tissues from exposed rats compared to samples from non-exposed animals. [1] Canistro, D.; Vivarelli, F.; Cirillo, S.; Babot Marquillas, C.; Buschini, A.; Lazzaretti, M.;Marchi, L.; Cardenia, V.; Rodriguez-Estrada, M.T.; Lodovici, M.; Cipriani, C.; Lorenzini, A.; Croco, E.; Marchionni, S.; Franchi, P.; Lucarini, M.; Longo, V.; Della Croce, C.M.; Vornoli, A.; Colacci, A.; Vaccari, M.; Sapone, A.; Paolini, M. SCIENTIFIC REPORTS. 2017, DOI:10.1038/s41598-017-02317-8 [2] Vivarelli, F.; Canistro, D.; Franchi, P.; Sapone, A.; Vornoli, A.; Della Croce, C.; Lucarini, M.; Paolini, M. Life Sciences, 2016, 145, 166-173. DOI:10.1016/j.lfs.2015.12.033 [3] Fabbri, R.; Sapone, A.; Paolini, M.; Vivarelli, F.; Franchi, P.; Lucarini, M.; Pasquinelli, G.; Vicenti, R.; Macciocca, M.; Venturoli, S.; Canistro, D. Hystology and Hystopatology, 2015, 30, 725-730 DOI: 10.14670/HH-30.725
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- 2017
9. E-cigarettes induce toxicological effects that can raise the cancer risk. A frame from drug-metabolism and antioxidant homeostasis
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CANISTRO D., VIVARELLI F., CIRILLO S., CARDENIA V., RODRIGUEZ-ESTRADA M. T., PAOLINI M., Canistro, D., Vivarelli, F., Cirillo, S., Cardenia, V., RODRIGUEZ-ESTRADA, M. T., and Paolini, M.
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E-cigarette, toxicological effects, rat - Abstract
E-CIGARETTES INDUCE TOXICOLOGICAL EFFECTS THAT CAN RAISE THE CANCER RISK. A FRAME FROM DRUG-METABOLISM AND ANTIOXIDANT HOMEOSTASIS. 1)Canistro D. 2)Vivarelli F. 3)Cirillo S. 4)Cardenia V. 5)Rodriguez-estrada MT. Dept of Pharmacy and Biotechnology, Unibo Electronic cigarettes (e-cigs) are devices designed to deliver nicotine in a vaping solution without tobacco combustion. Perceived as a safer alternative to conventional cigarettes, e-cigs are aggressively marketed as lifestyle-choice consumables, thanks to few restrictions and a lack of regulatory guidelines. Despite the burgeoning worldwide consumption of e-cigs, their safety remains largely unproven and it is unknown whether these devices cause in vivo toxicological effects that could contribute to cancer occurrence. In the present study, we investigated the co-mutagenic and cancer-initiating effects of e-cig vapour in a rat model. To explore whether e-cigs induce toxicological effects, such as those involving cytochrome P450 (CYP) changes, we analyzed the modulation of carcinogen metabolizingenzymes in the lung of rats exposed to e-cig vapour. We observed a significant increase in CYP1A1/2 (activating, for example, polychlorinated biphenyls, aromatic amines, dioxins and PAHs), CYP2B1/2 (activating olefins and halogenated hydrocarbons), 2C11 (activating nitrosamines and mycotoxins) and CYP3A (activating hexamethyl phosphoramide and nitrosamines) documented by the sharp rise in the corresponding probes. Conversely, we observed that the antioxidant enzymes catalase, DT-diaphorase and glutathione peroxidase and the conjugating phase II glutathione S-transferases, mainly involved in xenobiotic detoxification, were noticeable decreased, whereas UDP-glucuronyl-transferase was substantially unchanged. Extrapolated to humans, the corresponding boosted CYP-linked monooxygenases together with reduced activity of antioxidant and detoxifying machinery would predispose a subject to an enhanced cancer risk from the widely bioactivated e-cig vapour procarcinogens associated with an increased risk of lung cancer.
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- 2017
10. Development of microparticles for oral administration of the non-conventional radical scavenger IAC and testing in an inflammatory rat model
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CIRILLO S., PAOLINI M., VIVARELLI F., PASSERINI N., ALBERTINI B., DI SABATINO M., CORACE G., LUPPI B., CANISTRO D., Cirillo, S., Paolini, M., Vivarelli, F., Passerini, N., Albertini, B., DI SABATINO, M., Corace, G., Luppi, B., and Canistro, D.
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Microparticles, radical scavenger, Inflammation, rat - Abstract
Development of microparticles for oral administration of the non-conventional radical scavenger IAC and testing in an inflammatory rat model 1)Cirillo S.. 2)Paolini M.. 3)Vivarelli F.. 4)Passerini N.. 5)Albertini B.. 6)Di sabatino M. 7)Corace G.. 8)Luppi B.. 9)Canistro D.. University of Bologna The bis (1-hydroxy-2,2,6,6-tetramethyl-4-piperidinyl)-decandioate (IAC) is an innovative nonconventional radical scavenger used with success in several disease models, such as inflammation, neurological disorders, hepatitis and diabetes. To date, the main limit for the drug use is represented by the intraperitoneal (i.p.) route of administration used in the pharmacological treatments. In order to develop a delivery system that allowed both oral administration and the therapeutic efficacy, Solid Lipid Microparticles (SLMs) containing a theoretical 18% w/w of IAC have been produced. Recently, three formulations (A, B, C) have been tested at different dosages in an inflammation and pain rat model. Inflammatory model was induced by the use of an intraplantar injection of 100ml/paw of Freund's complete adjuvant (FCA). Administered per os at different dosages, IAC B (60% stearic acid-20% Compritol® HD5 ATO) was the most efficient formulation in reducing oedema and alleviating pain, compared to the gold standard Paracetamol. Since the anti-diabetic effects of the i.p. formulation of IAC was already demonstrated in vivo, we are now investigating the therapeutic efficacy of the selected (B) oral IAC formulation (SLMs) in streptozotocin-nicotinamide diabetic mice.
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- 2017
11. The chemopreventive effects of isothiocyanate moringin isolated from Moringa oleifera seeds
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VIVARELLI F., M. PAOLINI, C. , MICHL, A. RASCLE, J. , WEIGL, G. DE NICOLA, R. IORI, S. CIRILLO, D. CANISTRO, Vivarelli, F., Paolini, M., Michl, C., Rascle, A., Weigl, J., DE NICOLA, G., Iori, R., Cirillo, S., and Canistro, D.
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Moringa oleifera seeds, chemoprevention - Abstract
The chemopreventive effects of isothiocyanate moringin isolated from Moringa oleifera seeds 1)Vivarelli F. 2)Paolini M. 3)Michl C. 4)Rascle A. 5)Weigl J. 6)De nicola G. 7)Iori R. 8)Cirillo S. 9)Canistro D. University of Bologna Over the past years, there has been a growing interest in the natural constituents of vegetables as a potential means of cancer control. Isothiocyanates (ITCs) are considered as ideal chemopreventive agents, due to their abundance in easily accessible brassica vegetables, their ability to target multiple pathways involved in cancer aetiology coupled with a favourable toxicological profile. Recently it was reported that sulphoraphane (SFN) inhibits STAT5-mediated transcription. STAT5 (Signal Transducer and Activator of transcription 5) belongs to a family of transcription factors (STAT1-6) mainly present in an inactive form in the cytoplasm of numerous cell types and which are activated by phosphorylation in response to specific cytokines hormones and growth factors. STAT5 plays a key role in the control of cell proliferation and survival, via the regulation of genes such as c-Myc, Pim-1, Bcl-x, Osm or Cis and it also contributes to immune cell differentiation and function. Its activity is normally tightly controlled, and is hence frequently found deregulated in cancer where it is often constitutively activated. For these reasons STAT inhibitors are considered as potential candidates for cancer prevention or therapy. Beside SFN, more recently the isothiocyanate moringin (GMG-ITC), isolated from the Moringa oleifera, has caught the interest of scientific community for its anti-inflammatory activity through the inhibition of the NF-κ B pathway and it showed interesting anti cancer effects against mouse multiple myeloma and human astrocytoma cell line. However, till now, very little is known about the activity of GMG-ITC on cell signaling pathways. The present study was conceived to explore the potential inhibitory effect of GMG-ITC on crucial pathways commonly up-regulated in cancer, such as JAK/STAT and NF-κB comparing results with those obtained with SFN. Results showed how SFN and GMG-ITC were able to suppress IL-3- induced expression of STAT5 target genes in mouse pro-B cells, however, GMG-ITC reported a stronger inhibitory activity compared to SFN. Both GMG-ITC and SFN did not inhibit STAT5 phosphorylation, suggesting a downstream inhibitory event. Expression of interferon (IFNα)- stimulated STAT1/STAT2 target genes (G1P3, ISG15, STAT1, IRF9) in HeLa cells were downregulated by GMG-ITC and SFN without altering STAT1 and STAT2 phosphorylation. Also in this case GMG-ITC exhibited a more marked activity then those observed with SFN. Notable, basal expression of c-Myc remained unaffected upon treatment with up to 10 μM SFN or GMG-ITC, indicating that both ITCs inhibit STAT5-induced but not basal c-Myc. GMG-ITC and SFN had a limited effect on IFNα-induced STAT1 and STAT2 activity, indicating that both ITCs differentially target JAK/STAT signaling pathways. Furthermore, we showed that GMG-ITC in the micromolar range is a more potent inhibitor of TNF-induced NF-κB activity than SFN. TNF-induced expression of IL-8 and IL-6 was inhibited by both SFN and GMG-ITC, but this last appeared to be more effective. Interestingly, SFN and GMG-ITC inhibit NF-κ B signaling with a greater potency than that mediated by the well-known NF-κB inhibitor curcumin. As a whole, our data indicate how GMGITC could be considered as a potent inhibitor of STAT5, NF-κ B as well as STAT1/STAT2 signaling pathways, often overcoming the effects obtained with SFN. Given the implication of these pathways in the carcinogenesis, inflammatory diseases and immune disorders, GMG-ITC could represent a newsworthy and attractive chemopreventive agent.
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- 2017
12. Effects of electronic cigarette vapors exposure on oxidative damage and antioxidant status
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E. BIGAGLI, CANISTRO D., PAOLINI M., VIVARELLI F., CIRILLO S., LODOVICI, MAURA, Bigagli, E., Canistro, D., Paolini, M., Vivarelli, F., Cirillo, S., and Lodovici, M.
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E-cigarette, oxidative damage, antioxidant status - Abstract
Effects of electronic cigarette vapors exposure on oxidative damage and antioxidant status. 1)Bigagli E. 2)Canistro D. 3)Paolini M. 4)Vivarelli F. 5)Cirillo S. 6)Lodovici M. 1)Neurofarba, University of florence, Florence, Italy 2)Farmacia e biotecnologie, University of bologna, Bologna, Italy 3)Farmacia e biotecnologie, University of bologna, Bologna, Italy 4)Farmacia e biotecnologie, University of bologna, Bologna, Italy 5)F Electronic cigarettes (e-cigs) are devices designed to deliver nicotine without burning tobacco and therefore, they are perceived as a safer alternative to the conventional cigarettes. However, because of the high temperature reached by e-cig solutions (> 200 C°) many toxic substances, including polycyclic aromatic hydrocarbons, formaldehyde, nitrosamines, metals and carbonyls can be generated. Very few in vivo animal studies have been conducted so far, most of them based on short-term e-cig exposure. The aim of this study was therefore to evaluate the influence of e-cigs on oxidative stress related parameters, classical markers associated to conventional cigarette toxicity. Male Sprague Dawley rats (8 weeks of age), were housed in an inhalation chamber and exposed either to e- cig vapors (1 mL/day of e-liquid containing 18 mg/mL of nicotine) or to a saline solution. One cycle of treatment consisted in 17 sec puff, 6 sec on, 5 sec off, 6 sec on, followed by 20 minutes stop. e-cigs voltage was set at 5.5. Animals were submitted to 11 cycles/ day for 5 consecutive days/week, for 4 consecutive weeks. At sacrifice, liver, kidneys, lungs, bladder and plasma were collected for the analysis of protein (carbonyl residues) and DNA oxidative damage (8-hydroxy-2’-deoxyguanosine (8-OHdG)) and of the total antioxidant power (FRAP assay). At lung level, we found that FRAP values of rats exposed to e-cigs vapors were markedly reduced compared to controls. A similar trend was observed in the plasma, even if the statistical significance was not reached. Plasma FRAP levels and carbonyl residues were inversely correlated in e-cig exposed rats but not in controls. We also found that 8-OHdG markedly increased in the lung of e-cig vapor exposed rats compared to controls. An inverse correlation between FRAP levels and 8-OHdG in lung tissue from exposed animals was also observed. These results demonstrate that e-cig vapor causes DNA oxidative damage and impairs antioxidant defenses in rats; given that these toxicological outcomes are typically induced by conventional cigarettes smoking, further investigations to better identify harmful e-cig effects especially in the long term, are of paramount importance.
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- 2017
13. Raphanus sativus cv. Sango sprout juice decreases diet-induced obesity in sprague dawley rats and ameliorates related disorders
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Vivarelli, F, Canistro, D, Sapone, A, De Nicola, G, Marquillas, C, Iori, R, Antonazzo, I, Gentilini, F, Paolini, M, Vivarelli F., Canistro D., Sapone A., De Nicola G. R., Marquillas C. B., Iori R., Antonazzo I. C., Gentilini F., Paolini M., Vivarelli, F, Canistro, D, Sapone, A, De Nicola, G, Marquillas, C, Iori, R, Antonazzo, I, Gentilini, F, Paolini, M, Vivarelli F., Canistro D., Sapone A., De Nicola G. R., Marquillas C. B., Iori R., Antonazzo I. C., Gentilini F., and Paolini M.
- Abstract
Background Obesity is recognized as a leading global health problem, correlated with an increased risk for several chronic diseases. One strategy for weight control management includes the use of vegetables rich in bioactive compounds to counteract weight gain, improve the antioxidant status and stimulate lipid catabolism. Aim of the Study The aim of this study was to investigate the role of Raphanus sativus Sango sprout juice (SSJ), a Brassica extraordinarily rich in anthocyanins (AC) and isothiocyanates (ITCs), in a non-genetic model of obesity (high fat diet-HFD induced). Methods Control groups were fed with HFD or regular diet (RD). After a 10-week period, animals were assigned to experimental units and treated by gavage for 28 days as follows: HFD and RD control groups (rats fed HFD or RD and treated with vehicle only) and HFD-treated groups (rats fed HFD and treated with 15, 75 or 150 mg/kg b.w. of SSJ). Body weight and food consumption were recorded and serum lipid profile was measured (total cholesterol, triglycerides, and non-esterified fatty acids). Hepatic phase-I, phase-II as well as antioxidant enzymatic activities were assessed. Results SSJ lowered total cholesterol level, food intake and liver weight compared with HFD rodents. SSJ at medium dose proved effective in reducing body-weight (~19 g reduction). SSJ was effective in up-regulating the antioxidant enzymes catalase, NAD(P)H:quinone reductase, oxidised glutathione reductase and superoxide dismutase, which reached or exceeded RD levels, as well as the phase II metabolic enzyme UDP-glucuronosyl transferase (up to about 43%). HFD up-regulated almost every cytochrome P450 isoform tested, and a mild down-regulation to baseline was observed after SSJ intervention. Conclusion This work reveals, for the first time, the antioxidant, hypolipidemic and antiobesity potential of SSJ, suggesting its use as an efficient new functional food/nutraceutical product.
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- 2016
14. Scavenging of gases during growth of ice crystals
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Santachiara, G., primary, Prodi, F., additional, and Vivarelli, F., additional
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- 1995
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15. Surveying & maintaining the Transmed pipeline
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Louaar, A. and Vivarelli, F.
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TMPC Inc. -- Management ,Natural gas ,Pipe lines -- Maintenance and repair ,Business ,Petroleum, energy and mining industries - Abstract
TMPC Inc built the 106-mile underwater portion of the Algeria-to-Italy Transmed gas pipe line through the Sicilian Channel. The project was completed in 1981; however, the company continues to have responsibility for its inspection and maintenance. TMPC utilizes new technologies as they evolve to manage the undersea pipe lines. The pipe lines and coastal landing points are inspected visually and by instrument each year, with cathodic protection surveys every five years. If serious problems are detected, they are fixed immediately. Additional maintenance is done as needed.
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- 1992
16. Ameliorative potential of Raphanus Sativus cv. Sango sprout juice in obese rats maintained with high fat diet or switched to regular diet
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VIVARELLI F., D. CANISTRO, A. SAPONE, G. R. DE NICOLA, C. BABOT MARQUILLAS, R. IORI, F. GENTILINI, M. PAOLINI, Vivarelli, F., Canistro, D., Sapone, A., DE NICOLA, G. R., BABOT MARQUILLAS, C., Iori, R., Gentilini, F., and Paolini, M.
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food and beverages ,Obesity, Raphanus Sativus Sango, rata - Abstract
Ameliorative potential of Raphanus sativus cv. Sango sprout juice in obese rats maintained with high fat diet or switched to regular diet F. Vivarelli1, D. Canistro1, A. Sapone1, G.R. De Nicola2, C. Babot Marquillas1, R. Iori2, F. Gentilini3, M. Paolini1 1Dept. of Pharmacy and Biotechnology, Alma Mater Studiorum-University of Bologna, Via Irnerio 48, 40126, Bologna, Italy 2Industrial Crop Research Centre, Agricultural Research Council, (CRA-CIN), Via di Corticella, 133, 40128, Bologna, Italy 3Dept. of Veterinary Medical Sciences, Alma Mater Studiorum-University of Bologna, via Tolara di Sopra 50, 40064, Ozzano dell'Emilia, Bologna, Italy Obesity is a worldwide epidemic characterized not only by excessive fat deposition but also by systemic low grade of inflammation and high oxidative stress. Despite much progress has been achieved in recent years, current pharmacological approaches for long-term therapy offer modest benefits for most patients. The present study evaluated the ameliorative effect of Raphanus sativus Sango sprout juice (SSJ), a Brassica extraordinarily rich in anthocyanins (AC) and isothiocyanates (ITCs), in a non-genetic model of obesity (high fat diet-HFD induced). Rats were fed with HFD or regular diet (RD); after 10-weeks, the HFD animals were assigned to four experimental units and the interventional period was 28 days long: 1) HFD-RD, the diet switched from HFD to RD and received the vehicle only; 2) HFD+SSJ and 3) HFD-RD+SSJ, treated with 75 mg/kg b.w. of SSJ; 4) HFD and 5) RD vehicle only, controls. Our model of obesity showed hyperlipidaemia as well as a marked increase of body and liver weight. The transition from HFD to RD, as expected, led to a significant loss of excess weight (-9.83 g; p
- Published
- 2015
17. Effetti del germoglio di Raphanus Sativus CV Sango in un modello animale di obesità
- Author
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VIVARELLI F., D. CANISTRO, A. SAPONE, C. BABOT MARQUILLAS, G. R. DE NICOLA, R. IORI, I. C. ANTONAZZO, F. GENTILINI, M. PAOLINI, Vivarelli, F., Canistro, D., Sapone, A., BABOT MARQUILLAS, C., DE NICOLA, G. R., Iori, R., Antonazzo, I. C., Gentilini, F., and Paolini, M.
- Subjects
Obesity, Raphanus Sativus Sango, rat - Abstract
Effetti del germoglio di Raphanus Sativus CV Sango in un modello animale di obesità F. Vivarelli1, D. Canistro1, A. Sapone1, C. Babot Marquillas1, G.R. De Nicola2, R. Iori2, I.C. Antonazzo1, F. Gentilini3 e M. Paolini1. 1 Unità di Tossicologia Molecolare, Dipartimento di Farmacia e Biotecnologie, Alma Mater Studiorum, Università di Bologna, 40127 Bologna, Italia. 2 Consiglio per la Ricerca e la Sperimentazione in Agricoltura, Centro di Ricerca per le Colture Industriali (CRA-CIN), 40128 Bologna, Italia. 3 Dipartimento di Scienze Mediche Veterinarie, Alma Mater Studiorum, Università di Bologna, 40064 Ozzano dell’Emilia, Bologna, Italia. L’Organizzazione Mondiale della Sanità (OMS) ha riconosciuto l’obesità come un’epidemia globale, che costituisce uno dei principali problemi concernenti la salute pubblica, essendo un importante fattore di rischio per varie malattie croniche, come il diabete mellito di tipo 2, malattie cardiovascolari, patologie endocrine e tumori. Evidenze scientifiche sostengono l’ipotesi che alcuni alimenti o derivati abbiano effetti benefici sulla salute e, ad oggi, la corretta nutrizione è considerata un valido strumento di prevenzione per numerose patologiche. E’ noto, come l’obesità influenzi lo status ossidativo, determinando un’anomala produzione di specie reattive dell’ossigeno (ROS), condizione che frequentemente viene esacerbata da una deplezione delle comuni difese antiossidanti a livello cellulare. Diversi vegetali appartenenti alla famiglia delle Brassicaceae, contenenti elevate concentrazioni di glucosinolati (GLs) e isotiocianati (ITCs), hanno attirato l’interesse della comunità scientifica per le loro proprietà ipolipemizzanti e antiossidanti, come evidenziato dal crescente numero di studi preclinici ed epidemiologici. Scopo di questo lavoro è stato quello di indagare gli effetti del succo di germoglio di Raphanus Sativus Sango (SSJ), una Brassicacea straordinariamente ricca in antocianine (AC) e GLs, in un modello animale non genetico di obesità. La patologia è stata indotta sottoponendo ratti del ceppo Sprague Dawley a una dieta iperlipidica (HFD) per 10 settimane consecutive; al gruppo di controllo è stata assegnata una dieta standard (RD). Tre differenti dosaggi (15, 75 o 150 mg/kg p.c.) di SSJ sono stati somministrati per os per 28 giorni consecutivi; durante la fase di intervento, ai relativi gruppi di controllo (HFD e RD) è stato somministrato un volume equivalente del veicolo (acqua). I risultati mostrano una significativa riduzione del peso corporeo nei gruppi trattati con il dosaggio più basso (body weight gain = -0.29 g, p
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- 2015
18. Sickle-Cell Anaemia
- Author
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Mackey, J. P. and Vivarelli, F.
- Published
- 1954
19. Effect of Vitamin E supplementation on xenobiotic-metabolizing and antioxidant enzymes in rat
- Author
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VIVARELLI F., D. CANISTRO, A. SAPONE, S. FILIPPI, I. C. ANTONAZZO, C. BABOT MARQUILLAS, M. PAOLINI, Vivarelli, F., Canistro, D., Sapone, A., Filippi, S., Antonazzo, I. C., BABOT MARQUILLAS, C., and Paolini, M.
- Subjects
Vitamin E, xenobiotic metabolizing enzymes, rat - Abstract
Effect of Vitamin E supplementation on xenobiotic-metabolizing and antioxidant enzymes in rat. F. Vivarelli1 D. Canistro1, A. Sapone1, S. Filippi2, I.C. Antonazzo1, C. Babot Marquillas1 M. Paolini1 1 Molecular Toxicology Unit, Department of Pharmacy and Biotechnology, Alma-Mater Studiorum, University of Bologna, 40127 Bologna, Italy. 2 Interdepartmental Laboratory of Functional and Cellular Pharmacology of Reproduction, Department of NEUROFARBA and Department of Experimental, Clinical and Biomedical Sciences, University of Florence, 50139 Florence, Italy. Since its discovery and isolation Vitamin E (VE) has been considered a “safe” agent. VE has a number of biological functions being the antioxidant one, as peroxyl radical scavenger, the best known. The relationship between VE and cancer risk has been investigated in epidemiological studies and clinical trials with conflicting results. Recently, Selenium and Vitamin E Cancer Prevention Trial (SELECT) unexpectedly showed an increased risk of all primary cancers among healthy man supplemented with VE. As the literature reports that VE induce the P450 in human hepatoma cell line (HepG2), and being also known that such induction is always linked to an increased free radical and metabolite generation (cocarcinogenesis), we hypothesized that a generalized CYP upregulation migth have a role in the SELECT outcomes. Sprague Dawley male rats were intraperitoneally daily treated (for 7 or 14 consecutive days) with VE (α-tocopherol) at 100 or 200 mg/kg b.w. doses. The putative effects of VE on hepatic and renal microsomal CYP-linked monooxygenases as well as on antioxidant and post-oxidative enzymes were investigated. The almost neutral effect exerted by VE on hepatic phase I and II xenobiotic metabolizing enzymes, and the appreciable increase of catalase (up to 73% after 7 day treatment at lowest dose, p
- Published
- 2014
20. Positive Selection and Gene Conversion Drive the Evolution of a Brain-Expressed snoRNAs Cluster
- Author
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Ogorelkova, M., primary, Navarro, A., additional, Vivarelli, F., additional, Ramirez-Soriano, A., additional, and Estivill, X., additional
- Published
- 2009
- Full Text
- View/download PDF
21. ANTIBIOTICOTERAPIA EMPIRICA NEL BAMBINO NEUTROPENICO: ESPERIENZA CON CEFTRIAXONE + AMIKACINA VS AZLOCILLINA + AMIKACINA
- Author
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Bontempi, N., Bollettini, S., Branchini, M., Zanna, B., Vivarelli, F., Vecchi, V., Rosito, P., and Paolucci, Paolo
- Subjects
ANTIBIOTICOTERAPIA EMPIRICA ,BAMBINO NEUTROPENICO ,CEFTRIAXONE + AMIKACINA VS AZLOCILLINA + AMIKACINA - Published
- 1990
22. Bayesian neural network for fermentation control
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Vivarelli, F., primary, Serra, R., additional, Agagliati, E., additional, Malcangi, A., additional, and Muraca, R., additional
- Published
- 2000
- Full Text
- View/download PDF
23. Using Bayesian neural networks to classify segmented images
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Vivarelli, F., primary
- Published
- 1997
- Full Text
- View/download PDF
24. Scavenging of SO2 and HCl during growth of ice crystals by vapour diffusion
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Santachiara, G., primary, Prodi, F., additional, and Vivarelli, F., additional
- Published
- 1995
- Full Text
- View/download PDF
25. Further experiments on SO2 oxidation rate in monodisperse droplets grown on carbon nuclei in presence of O2 and NO2
- Author
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Santachiara, G, primary, Prodi, F, additional, and Vivarelli, F, additional
- Published
- 1993
- Full Text
- View/download PDF
26. Characteristics of atmospheric particles (airborne and in snowpack)at Khumbu glacier in the Nepalese Himalayas (EV-K2-CNR project)
- Author
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Vivarelli, F., primary, Santachiara, G., additional, and Prodi, F., additional
- Published
- 1991
- Full Text
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27. Dry deposition measurements of aerosol particles in a corn field
- Author
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Santachiara, G., primary, Prodi, F., additional, and Vivarelli, F., additional
- Published
- 1991
- Full Text
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28. SO2 oxidation in monodisperse droplets grown on carbon nuclei in presence of NO2
- Author
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Santachiara, G., primary, Prodi, F., additional, and Vivarelli, F., additional
- Published
- 1990
- Full Text
- View/download PDF
29. Comparing Bayesian neural network algorithms for classifying segmented outdoor images
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Vivarelli, F. and Williams, C. K.
- Published
- 2001
- Full Text
- View/download PDF
30. IL BAMBINO CON NEOPLASIA
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Vecchi, V., Pession, A., Serra, L., Butturini, A., Rosito, P., Mancini, A. F., Vivarelli, F., and Paolucci, Paolo
- Subjects
età evolutiva ,tumori - Published
- 1983
31. Prognostic significance of lymphoblast morphology in acute lymphoblastic leukaemia (ALL) in childhood
- Author
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Antonia Mancini, Pasquale Rosrro, Andrea Pession, Guido Paolucci, Vivarelli F, and Vico Vecchi
- Subjects
business.industry ,Lymphoblast ,Age Factors ,Morphology (biology) ,Hematology ,medicine.disease ,Prognosis ,Leukemia, Lymphoid ,Leukemia ,Child, Preschool ,Cancer research ,Medicine ,Lymphoblastic leukaemia ,Humans ,Lymphocytes ,business ,Child - Published
- 1980
32. Neuroblastoma in a pair of identical twins
- Author
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Guido Paolucci, R. Vallicelli, Giacomo Faldella, Laura Serra, Vivarelli F, Vico Vecchi, Antonia Mancini, and Pasquale Rosito
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Male ,Cancer Research ,Cell type ,Pathology ,medicine.medical_specialty ,Urology ,Adrenal Gland Neoplasms ,Twins ,Neuroblastoma ,Pregnancy ,Tumor regression ,Diseases in Twins ,Medicine ,Humans ,Family history ,Fetal Death ,Fetus ,business.industry ,Liver Neoplasms ,Clinical course ,Infant ,Twins, Monozygotic ,medicine.disease ,Prognosis ,Primary tumor ,Pedigree ,Oncology ,Pediatrics, Perinatology and Child Health ,Female ,business ,Identical twins ,Hereditary Neuroblastoma - Abstract
Hereditary neuroblastoma in a pair of identical twins is reported. In one of the twins the tumor occurred in fetal life and caused death of the twin before birth; in the other one, the tumor occurred at two months of life as IV-S neuroblastoma in the liver with primary tumor undetected. The unusual clinical course of the latter case is described: twice there was tumor regression, but in spite of treatment, fatal uncontrolled growth occurred. The family history, characterized by neoplasms of dissimilar cell types but without additional cases of neuroblastoma, is also detailed.
- Published
- 1982
33. Childhood non-Hodgkin's lymphoma and 'leukemia-lymphoma syndrome': long-term results with the modified LSA2-L2 protocol
- Author
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Vico Vecchi, Roberta Burnelli, Vivarelli F, Guido Paolucci, Andrea Pession, Laura Serra, Antonia Mancini, Pasquale Rosito, and Paolo Paolucci
- Subjects
non-Hodgkin's lymphoma ,medicine.medical_specialty ,medicine.medical_treatment ,Gastroenterology ,Central nervous system disease ,leukemia-lymphoma syndrome ,Diagnosis, Differential ,hemic and lymphatic diseases ,Internal medicine ,Antineoplastic Combined Chemotherapy Protocols ,Medicine ,LSA2-L2 protocol ,Humans ,Life Tables ,Stage (cooking) ,Child ,Survival rate ,Cyclophosphamide ,business.industry ,Lymphoma, Non-Hodgkin ,Lymphoblastic lymphoma ,Daunorubicin ,Hematology ,Syndrome ,Precursor Cell Lymphoblastic Leukemia-Lymphoma ,medicine.disease ,Prognosis ,Combined Modality Therapy ,Lymphoma ,Surgery ,Radiation therapy ,Survival Rate ,Regimen ,medicine.anatomical_structure ,Methotrexate ,Oncology ,Italy ,Evaluation Studies as Topic ,Vincristine ,Pediatrics, Perinatology and Child Health ,Prednisone ,Bone marrow ,Cranial Irradiation ,business - Abstract
From June 1976 to December 1984, 48 previously untreated children with non-Hodgkin's lymphoma (NHL) were treated according to the LSA2-L2 protocol, modified by inclusion of cranial irradiation for patients in stage III and stage IV disease. According to the staging system proposed by Wollner, 4 patients were in stage I, 8 in stage II, 11 in stage III, 8 in stage IVA (less than or equal to 25% blasts in the bone marrow), 15 in stage IVB (greater than 25% blasts in the bone marrow), and 2 in stage IV central nervous system disease. The complete remission rate was 95.8%. The relapse-free survival (RFS) rate of 46 complete responders was 76% after a median observation time of 47+ months. Only 1 of 35 high-risk responder patients developed CNS relapse after prophylactic treatment. Clinical stages were related to the RFS: 100% in stage I-II vs. 69% in stage III-IV. All 8 patients in stage IV were alive without evidence of disease with a median observation time of 59+ months. Fifteen patients in stage IVB who had leukemia-lymphoma syndrome attained 59% RFS with a median observation time of 39+ months. After a median observation time of 38+ months, 29 of 37 patients are off therapy. The results emphasize the value of both the histologic and immunologic features and the stage of disease in predicting the outcome of NHL in children. The LSA2-L2 regimen appears to be a very effective protocol for children with lymphoblastic lymphoma, although it may be less efficacious for patients with large bone marrow involvement.
- Published
- 1986
34. Et si nous dansions ? / Jerry MENGO et son orchestre
- Author
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Wayne, Mabel (1904-1978). Auteur ou responsable intellectuel, Vivarelli, F.. Auteur ou responsable intellectuel, Tiomkin, Dimitri (1894-1979). Auteur ou responsable intellectuel, Spiers, Pierre (1917-1980). Auteur ou responsable intellectuel, Shuman, Mort (1936-1991). Auteur ou responsable intellectuel, Ruiz, Pablo Beltràn (1915-2008). Auteur ou responsable intellectuel, Powell, Mel (1923-1998). Auteur ou responsable intellectuel, Pomus, Doc (1925-1991). Auteur ou responsable intellectuel, Paté, André (1919-2000). Auteur ou responsable intellectuel, Pallavicini, Vito (1924-2007). Auteur ou responsable intellectuel, Ory, Kid (1890-1973). Auteur ou responsable intellectuel, Mengo, Jerry (1911-1979). Auteur ou responsable intellectuel, Gray, Jery. Auteur ou responsable intellectuel, Mengo, Jerry (1911-1979). Direction d'orchestre, Wayne, Mabel (1904-1978). Auteur ou responsable intellectuel, Vivarelli, F.. Auteur ou responsable intellectuel, Tiomkin, Dimitri (1894-1979). Auteur ou responsable intellectuel, Spiers, Pierre (1917-1980). Auteur ou responsable intellectuel, Shuman, Mort (1936-1991). Auteur ou responsable intellectuel, Ruiz, Pablo Beltràn (1915-2008). Auteur ou responsable intellectuel, Powell, Mel (1923-1998). Auteur ou responsable intellectuel, Pomus, Doc (1925-1991). Auteur ou responsable intellectuel, Paté, André (1919-2000). Auteur ou responsable intellectuel, Pallavicini, Vito (1924-2007). Auteur ou responsable intellectuel, Ory, Kid (1890-1973). Auteur ou responsable intellectuel, Mengo, Jerry (1911-1979). Auteur ou responsable intellectuel, Gray, Jery. Auteur ou responsable intellectuel, and Mengo, Jerry (1911-1979). Direction d'orchestre
- Abstract
Titre uniforme : [Ramona], Titre uniforme : [Ventiquattromila baci], Titre uniforme : [The unforgiven], Titre uniforme : [Muskrat ramble], Titre uniforme : [String of pearls], Comprend : Le bleu de l'été (The Green leaves of Summer) du film "Alamo" rock lent / Dimitri TIOMKIN - Non je ne regrette rien : slow rock / C. DUMONT - Les citrons de Tel Aviv : slow bounce / Pierre SPIER - La joie d'aimer ("The need for love") du film "Le Vent dans la plaine" ("The unforgiven") boléro / Dimitri TIOMKIN - Dix Mille bulles bleues ("Le mille bolle blu") cha cha rock / PALLAVICINI - QUE QUE QUE HAY : cha cha cha / René DENONCIN - Garde-moi la dernière danse : cha cha cha / D. POMUS et M. SHUMAN - Vingt-Quatre mille baisers ("Ventiquattromila baci") cha cha rock / VIVARELLI - MUSKRAT RAMBLE : dixieland-charleston / Kid ORY - AIN'T SHE SWEET ? : dixieland / M. AGER - ONE NIGHTER : slow bounce / Jerry MENGO - Tu peux... tu peux : medium / A. PATE - MY GUY'S COME BACK : medium / M. POWEL - A STRING OF PEARLS : fox bounce / J. GRAY - Ramona : cha cha cha / M. WAYNE - C'est si doux ("Quien sera") cha cha cha / P.B. RUIZ, BnF-Partenariats, Collection sonore - Believe, Contient une table des matières
- Published
- 1961
35. TROMPETTE D'OR : slow / G. JOUVIN et R. DENONCIN. RAMONA : moderato / Albert WILLEMETZ - Jean LE SEYEUX - Mabel WAYNE et L. WOLFEGILBERT. LE BLEU DE L'ETE : rock lent / Dimitri TIOMKIN. COU-COUCHE PANIER : cha cha cha / Serge CASTEL et René DENONCIN. LES MARRONS CHAUDS : cha cha cha / Cl. NICOLAS et G. GARVARENTZ. TU PARLES TROP : rock cha cha / JONES - Regina HOLL et G. ABER. FAUT RIGOLER : cha cha cha / Henri SALVADOR. ALLEZ SAVOIR POURQUOI : boléro cha cha / J.P. CALVET et J. BROUSSOLLE. ANNETTE, BRIGITTE ET Cie : cha cha cha / JOLLET - CANFORA et JOUVIN. 24.000 BAISERS : rock cha cha / Fernand BONIFAY - A. CELENTANO-FULCI et VIVARELLI. MON DIEU : slow / M. VAUCAIRE et Ch. DUMONT. LE PETIT CLOWN DE MON COEUR : moderato / Rudy REVIL - G. ABER - Pierre DELANOE - Don THIL et EVERLY. KILI WATCH : rock / JIL et JEAN et Gus DERSE. POUR FAIRE UN DIXIELAND : charleston / M. CASSEZ - Aimé BARELLI et G. GUSTIN ; Ray TCHICORAY et son Orchestre
- Author
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Willemetz, Albert (1887-1964). Auteur ou responsable intellectuel, Wayne, Mabel (1904-1978). Auteur ou responsable intellectuel, Vivarelli, F.. Auteur ou responsable intellectuel, Vaucaire, Michel (1904-1980). Auteur ou responsable intellectuel, Thil, Don. Auteur ou responsable intellectuel, Salvador, Henri (1917-2008). Auteur ou responsable intellectuel, Révil, Rudi (1916-1983). Auteur ou responsable intellectuel, Nicolas, Clément. Auteur ou responsable intellectuel, Leseyeux, Jean (18..-1957). Auteur ou responsable intellectuel, Jouvin, Georges (1923-2016). Auteur ou responsable intellectuel, Jones, Jo (1911-1985). Auteur ou responsable intellectuel, Jollet, Christian. Auteur ou responsable intellectuel, Holl, Regina. Auteur ou responsable intellectuel, Gustin, Gérard (1930-1995). Auteur ou responsable intellectuel, Gilbert, L. Wolfe (1886-1970). Auteur ou responsable intellectuel, Garvarentz, Georges (1932-1993). Auteur ou responsable intellectuel, Everly, Phil (1939-2014). Auteur ou responsable intellectuel, Derse, Gus. Auteur ou responsable intellectuel, Denoncin, René (1920-2002). Auteur ou responsable intellectuel, Delanoë, Pierre (1918-2006). Auteur du texte, Celentano, Adriano (1938-....). Auteur ou responsable intellectuel, Castel, Serge (1921-1981). Auteur ou responsable intellectuel, Cassez, Michel (1935-....). Parolier, Canfora, Armand (1921-1973). Auteur ou responsable intellectuel, Calvet, Jean-Pierre (1925-1989). Auteur ou responsable intellectuel, Broussolle, Jean (1920-1984). Auteur ou responsable intellectuel, Bonifay, Fernand (1920-1993). Auteur ou responsable intellectuel, Barelli, Aimé (1917-1995). Auteur ou responsable intellectuel, Tchicoray, Ray. Direction d'orchestre, Jil et Jan. Auteur ou responsable intellectuel, Willemetz, Albert (1887-1964). Auteur ou responsable intellectuel, Wayne, Mabel (1904-1978). Auteur ou responsable intellectuel, Vivarelli, F.. Auteur ou responsable intellectuel, Vaucaire, Michel (1904-1980). Auteur ou responsable intellectuel, Thil, Don. Auteur ou responsable intellectuel, Salvador, Henri (1917-2008). Auteur ou responsable intellectuel, Révil, Rudi (1916-1983). Auteur ou responsable intellectuel, Nicolas, Clément. Auteur ou responsable intellectuel, Leseyeux, Jean (18..-1957). Auteur ou responsable intellectuel, Jouvin, Georges (1923-2016). Auteur ou responsable intellectuel, Jones, Jo (1911-1985). Auteur ou responsable intellectuel, Jollet, Christian. Auteur ou responsable intellectuel, Holl, Regina. Auteur ou responsable intellectuel, Gustin, Gérard (1930-1995). Auteur ou responsable intellectuel, Gilbert, L. Wolfe (1886-1970). Auteur ou responsable intellectuel, Garvarentz, Georges (1932-1993). Auteur ou responsable intellectuel, Everly, Phil (1939-2014). Auteur ou responsable intellectuel, Derse, Gus. Auteur ou responsable intellectuel, Denoncin, René (1920-2002). Auteur ou responsable intellectuel, Delanoë, Pierre (1918-2006). Auteur du texte, Celentano, Adriano (1938-....). Auteur ou responsable intellectuel, Castel, Serge (1921-1981). Auteur ou responsable intellectuel, Cassez, Michel (1935-....). Parolier, Canfora, Armand (1921-1973). Auteur ou responsable intellectuel, Calvet, Jean-Pierre (1925-1989). Auteur ou responsable intellectuel, Broussolle, Jean (1920-1984). Auteur ou responsable intellectuel, Bonifay, Fernand (1920-1993). Auteur ou responsable intellectuel, Barelli, Aimé (1917-1995). Auteur ou responsable intellectuel, Tchicoray, Ray. Direction d'orchestre, and Jil et Jan. Auteur ou responsable intellectuel
- Abstract
Titre uniforme : [Ramona], Titre uniforme : [Ventiquattromila baci], BnF-Partenariats, Collection sonore - Believe, Contient une table des matières
- Published
- 1961
36. Intensification of induction prior to intensification of consolidation and bone marrow rescue in disseminated neuroblastoma
- Author
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Paolucci, P., Mancini, A. F., Rosito, P., Vecchi, V., Vivarelli, F., Donatella Granchi, Calzolari, P., and Paolucci, G.
- Subjects
Male ,Clinical Trials as Topic ,Neuroblastoma ,Child, Preschool ,Antineoplastic Combined Chemotherapy Protocols ,bone marrow transplantation ,neuroblastoma ,Humans ,Female ,Combined Modality Therapy ,Bone Marrow Transplantation
37. Absorption of sulfur dioxide on monodisperse water droplets and catalytic activity of carbon particles
- Author
-
Santachiara, G., primary, Prodi, F., additional, and Vivarelli, F., additional
- Published
- 1989
- Full Text
- View/download PDF
38. Neuroblastoma in a Pair of Identical Twins
- Author
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Mancini, A.F., primary, Rosito, P., additional, Faldella, G., additional, Serra, L., additional, Vallicelli, R., additional, Vecchi, V., additional, Vivarelli, F., additional, and Paolucci, G., additional
- Published
- 1982
- Full Text
- View/download PDF
39. Absorptionof sulfur dioxide on monodisperse water droplets and catalytic activity of carbon particles
- Author
-
Santachiara, G., Prodi, F., and Vivarelli, F.
- Published
- 1989
- Full Text
- View/download PDF
40. Digestibility, toxicity and metabolic effects of rapeseed and sunflower protein hydrolysates in mice
- Author
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Carlo Pinna, Monica Grandi, Luisa Ugolini, Emanuele Conte, Donatella Canistro, Luca Lazzeri, Giacomo Biagi, Silvia Cirillo, Fabio Vivarelli, Andrea Sapone, Ippazio Cosimo Antonazzo, Susanna Cinti, Canistro, D., Vivarelli, F., Ugolini, L., Pinna, C., Grandi, M., Antonazzo, I.C., Cirillo, S., Sapone, A., Cinti, S., Lazzeri, L., Conte, E., Biagi, G, Canistro, D, Vivarelli, F, Ugolini, L, Pinna, C, Grandi, M, Antonazzo, I, Cirillo, S, Sapone, A, Cinti, S, Lazzeri, L, and Conte, E
- Subjects
0301 basic medicine ,Rapeseed ,sunflower ,040301 veterinary sciences ,hydrolysate ,rapeseed ,Biology ,Hydrolysate ,0403 veterinary science ,03 medical and health sciences ,Mice ,Enzymatic hydrolysis ,study ,Palatability ,lcsh:SF1-1100 ,chemistry.chemical_classification ,toxicity ,04 agricultural and veterinary sciences ,Metabolism ,Sunflower ,030104 developmental biology ,Enzyme ,Biochemistry ,chemistry ,Toxicity ,Animal Science and Zoology ,lcsh:Animal culture ,protein - Abstract
The digestibility (in vitro), toxicity and metabolic effects of rapeseed (RPH) and sunflower (SPH) protein hydrolysates have been evaluated in a murine animal model. The enzyme AlcalaseVR was employed to obtain a mild enzymatic hydrolysis of rapeseed and sunflower defatted seed meals (DSM) protein isolates. Both hydrolysates showed higher in vitro digestibility than the respective DSM, presumably as a consequence of the hydrolysis process that they had undergone. In vivo, RPH and SPH were well tolerated. Body and organ weights, biochemical blood parameters from treated male mice were comparable to controls. Food intake was regular in RPH and SPH animals, suggesting a good palatability of the hydrolysates. Not relevant perturbations of the principal hepatic and renal drug metabolism enzymes were observed in RPH or SPH mice. In conclusion, protein hydrolysates from sunflower and rapeseed DSM did not determine relevant toxicological effects; therefore, they could be considered as alternative protein sources and/or food ingredients.
- Published
- 2017
41. Further experiments on SO 2 oxidation rate in monodisperse droplets grown on carbon nuclei in presence of O 2 and NO 2
- Author
-
Santachiara, G, Prodi, F, and Vivarelli, F
- Published
- 1993
- Full Text
- View/download PDF
42. Anticancer potential of allicin: A review
- Author
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Elena, Catanzaro, Donatella, Canistro, Valentina, Pellicioni, Fabio, Vivarelli, Carmela, Fimognari, Catanzaro E., Canistro D., Pellicioni V., Vivarelli F., and Fimognari C.
- Subjects
Pharmacology ,Biological Products ,Allicin ,Cytotoxicity ,food and beverages ,Pharmacokinetic ,Anticancer drug ,Sulfinic Acids ,Neoplasms ,Humans ,Selectivity ,Disulfides ,Garlic ,Cancer - Abstract
Phytochemicals have attracted attention in the oncological field because they are biologically friendly and have relevant pharmacological activities. Thanks to the intense and unique spicy aroma, garlic is one of the most used plants for cooking. Its consumption is correlated to health beneficial effects towards several chronic diseases, such as cancer, mainly attributable to allicin, a bioactive sulfur compound stored in different plant parts in a precursor form. The objective of this review is to present and critically discuss the chemistry and biosynthesis of allicin, its pharmacokinetic profile, its anticancer mechanisms and molecular targets, and its selectivity towards tumor cells. The research carried out so far revealed that allicin suppresses the growth of different types of tumors. In particular, it targets many signaling pathways associated with cancer development. Future research directions are also outlined to further characterize this promising natural product.
- Published
- 2022
43. The Customizable E-cigarette Resistance Influences Toxicological Outcomes: Lung Degeneration, Inflammation, and Oxidative Stress-Induced in a Rat Model
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Sabrina Burattini, Eleonora Turrini, Elisabetta Falcieri, Carmela Fimognari, Fabio Vivarelli, Moreno Paolini, Silvia Cirillo, Vladimiro Cardenia, Donatella Canistro, Marco B. L. Rocchi, Maria Teresa Rodriguez-Estrada, Cirillo S., Vivarelli F., Turrini E., Fimognari C., Burattini S., Falcieri E., Rocchi M.B.L., Cardenia V., Rodriguez-Estrada M.T., Paolini M., and Canistro D.
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0301 basic medicine ,Antioxidant ,DNA damage ,medicine.medical_treatment ,Resistance ,Inflammation ,Oxidative phosphorylation ,Pharmacology ,Toxicology ,medicine.disease_cause ,resistance ,03 medical and health sciences ,chemistry.chemical_compound ,0302 clinical medicine ,medicine ,oxidative stress ,Animal model ,Electronic cigarette ,Xanthine oxidase ,chemistry.chemical_classification ,Reactive oxygen species ,animal model ,inflammation ,030104 developmental biology ,chemistry ,Toxicity ,Oxidative stre ,medicine.symptom ,030217 neurology & neurosurgery ,Oxidative stress - Abstract
Despite the knowledge gap regarding the risk-benefit ratio of the electronic cigarette (e-cig), its use has grown exponentially, even in teenagers. E-cig vapor contains carcinogenic compounds (eg, formaldehyde, acetaldehyde, and acrolein) and free radicals, especially reactive oxygen species (ROS) that cause toxicological effects, including DNA damage. The role of e-cig voltage customization on molecule generation has been reported, but the effects of the resistance on e-cig emissions and toxicity are unknown. Here, we show that the manipulation of e-cig resistance influences the carbonyls production from nonnicotine vapor and the oxidative and inflammatory status in a rat model. Fixing the voltage at the conventional 3.5 V, we observed that the amount of the selected aldehydes increased as the resistance decreased from 1.5 to 0.25 Ω. Under these conditions, we exposed Sprague Dawley rats to e-cig aerosol for 28 days, and we studied the pulmonary inflammation, oxidative stress, tissue damage, and blood homeostasis. We found a perturbation of the antioxidant and phase II enzymes, probably related to the increased ROS levels due to the enhanced xanthine oxidase and P450-linked monooxygenases. Furthermore, frames from scanning electron microscope showed a disorganization of alveolar and bronchial epithelium in 0.25 Ω group. Overall, various toxicological outcomes, widely recognized as smoke-related injuries, can potentially occur in e-cig consumers who use low-voltage and resistance device. Our study suggests that certain “tips for vaping safety” cannot be established, and encourages further independent investigations to help public health agencies in regulating the e-cig use.
- Published
- 2019
- Full Text
- View/download PDF
44. Efficacy of a new delivery system based on solid lipid microparticles for the oral administration of the non-conventional antioxidant IAC on a diabetes mouse model
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Silvia Cirillo, Beatrice Albertini, Donatella Canistro, Moreno Paolini, Nadia Passerini, Antonio Soleti, Giulia Merizzi, Fabio Vivarelli, Canistro, D., Vivarelli, F., Cirillo, S., Soleti, A., Albertini, B., Passerini, N., Merizzi, G., and Paolini, M.
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Blood Glucose ,Male ,0301 basic medicine ,Antioxidant ,Endocrinology, Diabetes and Metabolism ,medicine.medical_treatment ,Administration, Oral ,030209 endocrinology & metabolism ,Solid lipid microparticles (SLMs) ,Pharmacology ,Diabete ,medicine.disease_cause ,Antioxidants ,Diabetes Mellitus, Experimental ,Random Allocation ,Mice ,03 medical and health sciences ,chemistry.chemical_compound ,Drug Delivery Systems ,0302 clinical medicine ,Endocrinology ,Oral administration ,Diabetes mellitus ,medicine ,Animals ,Humans ,Hypoglycemic Agents ,Particle Size ,Nicotinamide ,business.industry ,medicine.disease ,Streptozotocin ,Lipids ,Microspheres ,Treatment Outcome ,030104 developmental biology ,chemistry ,Basal (medicine) ,Oxidative stre ,Drug carrier ,business ,Oxidative stress ,medicine.drug - Abstract
Purpose: We previously showed the positive effects of the new antioxidant molecule bis(1-hydroxy-2,2,6,6-tetramethyl-4-piperidinyl)-decandioate (IAC) in reducing basal hyperglycaemia and relieving glucose intolerance in a diabetes model. However, the chemical properties of IAC did not allow an efficient oral administration, thus representing the main failing of that study. Here, we tested the effect of a new oral delivery system based on solid lipid microparticles (SLMs) in a diabetes mouse model. Methods: The diabetes model was induced in C57B1/6J mice using streptozotocin and nicotinamide. Only the animals that overcame the glycaemic threshold of 180 mg/dL were enrolled in the study. Diabetic animals were then randomly assigned to 4 groups (n = 9) and treated once a day for 5 consecutive weeks with IAC (50, 100, and 150 mg/kg b.w.). The control group was composed of (n = 7) healthy mice that received only the vehicle. Glucose level was weekly monitored during the treatment period and up to 3 weeks after the suspension of the treatment. Glucose tolerance and insulin-resistance test were carried out. Results: Our results showed that SLMs maintained the IAC effect in reducing basal hyperglycaemia as well as improving the insulin sensitivity and glucose tolerance. Conclusion: The present study confirms that SLMs are promising drug carriers, which allow the oral administration of IAC ensuring its therapeutic efficacy. The concrete possibility to administer IAC per os represents a significant breakthrough in the putative consideration of this multi-radical scavenger in the diabetes therapeutic approach.
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- 2018
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45. Co-carcinogenic effects of vitamin E in prostate
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Alessio Papi, Antonello Lorenzini, Silvia Cirillo, Marco Lucarini, Silvia Marchionni, Sandra Filippi, Enzo Spisni, Andrea Vornoli, Vincenzo Longo, Clara Della Croce, Donatella Canistro, Paola Franchi, Francesca Rotondo, Cristina Zanzi, Moreno Paolini, Fabio Vivarelli, Vivarelli F., Canistro D., Cirillo S., Papi A., Spisni E., Vornoli A., Croce C.M.D., Longo V., Franchi P., Filippi S., Lucarini M., Zanzi C., Rotondo F., Lorenzini A., Marchionni S., and Paolini M.
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Male ,0301 basic medicine ,medicine.medical_treatment ,medicine.disease_cause ,carcinogenesis, prostate ,Mice ,Prostate cancer ,0302 clinical medicine ,Cytochrome P-450 Enzyme System ,Prostate ,Vitamin E ,Multidisciplinary ,biology ,Chemistry ,3T3 Cells ,Up-Regulation ,Gene Expression Regulation, Neoplastic ,Cell Transformation, Neoplastic ,medicine.anatomical_structure ,Medicine ,DNA damage ,Science ,Article ,Cell Line ,03 medical and health sciences ,Benzo(a)pyrene ,medicine ,Animals ,Humans ,Micronuclei, Chromosome-Defective ,Carcinogen ,Gene Expression Profiling ,Prostatic Neoplasms ,Cancer ,Cytochrome P450 ,Neoplasms, Experimental ,medicine.disease ,Rats ,Oxidative Stress ,030104 developmental biology ,Risk factors ,Dietary Supplements ,Carcinogens ,biology.protein ,Cancer research ,Lipid Peroxidation ,Reactive Oxygen Species ,030217 neurology & neurosurgery ,Oxidative stress ,DNA Damage - Abstract
A large number of basic researches and observational studies suggested the cancer preventive activity of vitamin E, but large-scale human intervention trials have yielded disappointing results and actually showed a higher incidence of prostate cancer although the mechanisms underlying the increased risk remain largely unknown. Here we show through in vitro and in vivo studies that vitamin E produces a marked inductive effect on carcinogen-bioactivating enzymes and a pro-oxidant status promoting both DNA damage and cell transformation frequency. First, we found that vitamin E in the human prostate epithelial RWPE-1 cell line has the remarkable ability to upregulate the expression of various phase-I activating cytochrome P450 (CYP) enzymes, including activators of polycyclic aromatic hydrocarbons (PAHs), giving rise to supraphysiological levels of reactive oxygen species. Furthermore, our rat model confirmed that vitamin E in the prostate has a powerful booster effect on CYP enzymes associated with the generation of oxidative stress, thereby favoring lipid-derived electrophile spread that covalently modifies proteins. We show that vitamin E not only causes DNA damage but also promotes cell transformation frequency induced by the PAH-prototype benzo[a]pyrene. Our findings might explain why dietary supplementation with vitamin E increases the prostate cancer risk among healthy men.
- Published
- 2019
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46. Impairment of testicular function in electronic cigarette (e-cig, e-cigs) exposed rats under low-voltage and nicotine-free conditions
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Moreno Paolini, Fabio Vivarelli, Vladimiro Cardenia, Maria Teresa Rodriguez-Estrada, Silvia Cirillo, Donatella Canistro, Vivarelli F., Canistro D., Cirillo S., Cardenia V., Rodriguez-Estrada M.T., and Paolini M.
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0301 basic medicine ,Male ,medicine.medical_specialty ,Antioxidant ,medicine.medical_treatment ,Acetaldehyde ,DNA break ,Electronic Nicotine Delivery Systems ,medicine.disease_cause ,DNA breaks ,E-cigarette ,Formaldehyde ,Oxidative stress ,Testis ,030226 pharmacology & pharmacy ,General Biochemistry, Genetics and Molecular Biology ,Lipid peroxidation ,Rats, Sprague-Dawley ,03 medical and health sciences ,chemistry.chemical_compound ,0302 clinical medicine ,Electricity ,Internal medicine ,Lactate dehydrogenase ,medicine ,Animals ,General Pharmacology, Toxicology and Pharmaceutics ,Acrolein ,Carcinogen ,chemistry.chemical_classification ,Reactive oxygen species ,Chemistry ,DNA Breaks ,General Medicine ,Organ Size ,Rats ,Oxidative Stress ,030104 developmental biology ,Endocrinology ,Oxidative stre ,Smoking Cessation ,Volatilization ,Reactive Oxygen Species - Abstract
Despite the lack of knowledge of the effects of electronic cigarettes (e-cigarettes, e-cigs) on public health, they have been proposed as a part of smoking cessation efforts. Recently, several basic scientific studies have pointed out how e-cigs can generate carcinogens, such as e-cig liquid thermal degradation by-products, and how the exposure can lead to genomic damage through inhibiting DNA repair or disrupting the redox homeostasis. However, scientific studies have pointed out how e-cigs can generate carcinogens and their release could be avoided setting the device to a low-voltage regimen. To test this feasibility, we show the effects of e-cig vapour generated from a low-voltage device filled with a nicotine-free liquid on rat testicular functions. The chemical analysis revealed the presence of carbonyls, such as formaldehyde, acetaldehyde and acrolein. Rats exposed reported a lower relative testis weight and higher levels of lactate dehydrogenase (LDH) as tissue damage marker, along with an impairment of 3β-hydroxysteroid dehydrogenase (3β-HSD), 17β-hydroxysteroid dehydrogenase (17β-HSD) and glucose-6-phosphate dehydrogenase (G6PDH) as key enzymes in the steroidogenesis pathway. The pro-oxidative environment was confirmed by the higher amount of reactive oxygen species (ROS), the development of lipid peroxidation and protein carbonylation, as well as from the disruption of antioxidant capability. Finally, we observed a higher rate of DNA unwinding in white blood cell line and boosted lipoxygenase (LOX)-linked activity, a tumour promotion marker. Even with the device setting at weak conditions, our results if extrapolated to humans suggest that exposure to e-cig vapours might alter gonads function in male vapers.
- Published
- 2019
47. Surveying and maintaining the transmed pipeline
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Vivarelli, F [Mariconsult SpA, Milan (Italy)]
- Published
- 1992
48. Does the electronic-cigarette aerosol impact rat brain lipid profile?
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V. Cardenia, F. Vivarelli, S. Cirillo, D. Canistro, M. Paolini, M. T. Rodriguez-Estrada, ENOR, Cardenia, V., Vivarelli, F., Cirillo, S., Canistro, D., Paolini, M., and Rodriguez-Estrada, M. T.
- Subjects
Electronic cigarette, aerosol, rat brain, lipid profile, oxysterols ,lipid profile ,aerosol ,rat brain ,oxysterols ,Electronic cigarette - Abstract
The lack of tobacco combustion, the most attractive feature of electronic cigarettes (e-cigs), has quickly made these new devices become the most sought-after alternative to the traditional cigarettes, contributing also to its widespread safety perception. Contrary to the general belief that the electronic nicotine-delivery systems avoid the release of harmful chemicals, the high temperature reached by e-cig solutions can actually generate dozens of toxic compounds, some of which are listed as known human carcinogens. Male Sprague Dawley rats, at 8 weeks of age, were housed under a 12h-light/12h-dark cycle, 22°C, 60% humidity, and fed ad libitum. After 5 days’ adaptation, the rats were randomly split into two groups of 10 animals each (non-exposed (control group) and exposed). Animals were whole-body exposed to 11 cycles/day, in order to consume 1 mL/day of e-liquid containing 18 mg/mL of nicotine. At the end of each cycle, the animals were transferred to a clean chamber to begin the next one. Animals were treated 5 days/week for 4 consecutive weeks. Rats were fasted 16 h prior to sacrifice. Animals were anesthetized by administering Zoletil 100 (100 mg/kg b.w.) and then sacrificed by decapitation according to the approved Ministerial procedures. The rats’ brains were isolated and their lipid matter was subjected to the analysis of total fatty acids, sterols and oxysterols composition. The e-cig aerosol exposure decreased the total lipid content in rat brain. A slight increase of saturated fatty acids and n-6 long-chain polyunsaturated fatty acids (LC-PUFA) was detected, while n-3 LC-PUFA dropped. A reduction of total cholesterol content and its oxidation products was also observed; in fact, the levels of 7alfa-hydroxycholesterol, alfa/beta-epoxycholesterol isomers and triol were lower compared to those found in the control group. The present research study revealed how e-cigs aerosol could disrupt the lipid and cholesterol homeostasis in rat brain, which could contribute to the new occurrence of some neurodegenerative diseases. A deeper investigation is needed to assess the harmful health impact of e-cigs, particularly after long-term exposure.
- Published
- 2017
49. Disruption of redox homeostasis and carcinogen metabolizing enzymes changes by administration of vitamin E to rats
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Vincenzo Longo, Paola Franchi, Clara Della Croce, Donatella Canistro, Fabio Vivarelli, Marco Lucarini, Andrea Sapone, Moreno Paolini, Andrea Vornoli, Vivarelli, F, Canistro, D, Franchi, P, Sapone, A, Vornoli, A, Della Croce, C, Longo, V, Lucarini, M, and Paolini, M.
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0301 basic medicine ,Male ,Antioxidant ,medicine.medical_treatment ,Cytochrome P450 ,Phase II enzyme ,Pharmacology ,Kidney ,Free radical species ,General Biochemistry, Genetics and Molecular Biology ,Rats, Sprague-Dawley ,03 medical and health sciences ,Chemopreventive agent ,Cytochrome P-450 Enzyme System ,Phase II enzymes ,medicine ,Animals ,Anticarcinogenic Agents ,Vitamin E ,General Pharmacology, Toxicology and Pharmaceutics ,Carcinogen ,chemistry.chemical_classification ,biology ,Antioxidant enzyme ,General Medicine ,Monooxygenase ,Free radical specie ,030104 developmental biology ,Enzyme ,medicine.anatomical_structure ,chemistry ,Liver ,biology.protein ,Carcinogens ,Antioxidant enzymes ,Reactive Oxygen Species ,Oxidation-Reduction ,Drug metabolism - Abstract
Aims A large meta-analysis of randomized clinical trials has seriously questioned chemoprevention based on vitamins including vitamin E (VE), and an increased risk for cancer among long-term users was actually seen. However, the mechanism underlying these findings still remain unknown. To clarify the mechanism, in an in vivo model we studied the putative disruption of redox homeostasis and the perturbation of carcinogen metabolizing enzymes determined by VE. Main methods Male Sprague–Dawley rats were treated ip with either 100 or 200 mg/kg b.w. daily for 7 or 14 consecutive days. Controls received vehicle only. Cytochrome P450 (CYP) content, CYP-reductase, CYP-linked monooxygenases, as well as phase-II and the antioxidant enzymes catalase and NAD(P)H:quinone reductase were investigated in both liver and kidney. Free radical species in tissue subcellular preparations were measured by electronic paramagnetic resonance (EPR) spectroscopy coupled to a radical probe technique. Key findings No substantial changes of hepatic xenobiotic metabolism enzymes were determined by VE. Conversely, a powerful booster effect of various renal phase-I carcinogen bioactivating enzymes at both dosages and observational times was recorded. While no relevant changes of post-oxidative phase-II reactions were found in the liver, a significant inactivating effect was caused by VE in renal tissues. Antioxidant enzymes were found mainly downregulated by the treatment. In the kidney, a marked free radical over-generation linked to CYP induction was observed. Significance This study proved that VE acts as a co-carcinogen and pro-oxidant agent. Such epigenetic mechanisms may contribute to explain the harmful outcomes observed in humans.
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- 2016
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50. On Enzyme-Based Anticancer Molecular Dietary Manipulations
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Fabio Vivarelli, Andrea Sapone, Moreno Paolini, Ramona Moles, Donatella Canistro, Simone Melega, Sapone A., Canistro D., Melega S., Moles R., Vivarelli F., and Paolini M.
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Diet therapy ,lcsh:Biotechnology ,Health, Toxicology and Mutagenesis ,lcsh:Medicine ,Mutagenesis (molecular biology technique) ,Mutagen ,Review Article ,Biology ,medicine.disease_cause ,Models, Biological ,Xenobiotics ,chemistry.chemical_compound ,Nutrient ,lcsh:TP248.13-248.65 ,Neoplasms ,Detoxification ,Genetics ,medicine ,Animals ,Humans ,CANCER PREVENTION ,Molecular Biology ,Carcinogen ,chemistry.chemical_classification ,Evidence-Based Medicine ,business.industry ,lcsh:R ,General Medicine ,Diet ,Enzymes ,Biotechnology ,Enzyme ,chemistry ,DIETARY PHYTOCHEMICALS ,Molecular Medicine ,XENOBIOTIC METABOLISM ,business ,Xenobiotic ,Diet Therapy - Abstract
Evidence from both epidemiological and experimental observations has fuelled the belief that the high consumption of fruits and vegetables rich in nutrients and phytochemicals may help prevent cancer and heart disease in humans. This concept has been drastically simplified from the dietary approaches to the use of single bioactive components both as a single supplement or in functional foods to manipulate xenobiotic metabolism. These procedures, which aim to induce mutagen/carcinogen detoxification or inhibit their bioactivation, fail to take into account the multiple and paradoxical biological outcomes of enzyme modulators that make their effects unpredictable. Here, we show that the idea that the physiological roles of specific catalysts may be easily manipulated by regular long-term administration of isolated nutrients and other chemicals derived from food plants is not viable. In contrast, we claim that the consumption of healthy diets is most likely to reduce mutagenesis and cancer risk, and that both research endeavours and dietary recommendations should be redirected away from single molecules to dietary patterns as a main strategy for public health policy.
- Published
- 2012
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