8 results on '"Tirelli, Ezio"'
Search Results
2. Developmental differences in ethanol-induced sensitization using postweanling, adolescent, and adult Swiss mice
- Author
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Quoilin, Caroline, Didone, Vincent, Tirelli, Ezio, and Quertemont, Etienne
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- 2012
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3. Ontogeny of the stimulant and sedative effects of ethanol in male and female Swiss mice: gradual changes from weaning to adulthood
- Author
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Quoilin, Caroline, Didone, Vincent, Tirelli, Ezio, and Quertemont, Etienne
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- 2010
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4. Multi- and Transgenerational Outcomes of an Exposure to a Mixture of EndocrineDisrupting Chemicals (EDCs) on Puberty and Maternal Behavior in the Female Rat.
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López-Rodríguez, David, Aylwin, Carlos Francisco, Delli, Virginia, Sevrin, Elena, Campanile, Marzia, Martin, Marion, Franssen, Delphine, Gérard, Arlette, Blacher, Silvia, Tirelli, Ezio, Noël, Agnès, Lomniczi, Alejandro, and Parent, Anne-Simone
- Subjects
BIOLOGICAL models ,MATERNAL exposure ,DENTAL resins ,UREA ,ANIMAL experimentation ,INTERGENERATIONAL relations ,ACETAMINOPHEN ,PUBERTY ,GENETIC variation ,MOTHERHOOD ,PARENTING ,RATS ,PRENATAL exposure delayed effects ,PLASTICIZERS ,HYDROCARBONS ,CAMPHOR ,ADOLESCENCE ,HYPOTHALAMUS ,OVULATION ,ENVIRONMENTAL exposure ,ENDOCRINE disruptors ,EPIGENOMICS ,REPRODUCTIVE health ,PHENOTYPES - Abstract
BACKGROUND: The effects of endocrine-disrupting chemicals (EDCs) on fertility and reproductive development represent a rising concern in modern societies. Although the neuroendocrine control of sexual maturation is a major target of EDCs, little is known about the potential role of the hypothalamus in puberty and ovulation disruption transmitted across generations. OBJECTIVES: We hypothesized that developmental exposure to an environmentally relevant dose of EDC mixture could induce multi- and/or transgenerational alterations of sexual maturation and maternal care in female rats through epigenetic reprograming of the hypothalamus. We investigated the transmission of a disrupted reproductive phenotype via the maternal germline or via nongenomic mechanisms involving maternal care. METHODS: Adult female Wistar rats were exposed prior to and during gestation and until the end of lactation to a mixture of the following 13 EDCs: di-n-butyl phthalate (DnBP), di(2-ethylhexyl) phthalate (DEHP), bisphenol A (BPA), vinclozolin, prochloraz, procymidone, linuron, epoxynaxole, dichlorodiphenyldichloroethylene, octyl methoxynimmate, 4-methylbenzylidene camphor (4-MBC), butylparaben, and acetaminophen. Perinatally exposed offspring (F1) were mated with unexposed males to generate germ cell (F2) and transgenerationally exposed (F3 and F4) females. Sexual maturation, maternal behavior, and hypothalamic targets of exposure were studied across generations. RESULTS: Germ cell (F2) and transgenerationally (F3) EDC-exposed females, but not F1, displayed delayed pubertal onset and altered folliculogenesis. We reported a transgenerational alteration of key hypothalamic genes controlling puberty and ovulation (Kiss1, Esr1, and Oxt), and we identified the hypothalamic polycomb group of epigenetic repressors as actors of this mechanism. Furthermore, we found a multigenerational reduction of maternal behavior (F1–F3) induced by a loss in hypothalamic dopaminergic signaling. Using a cross-fostering paradigm, we identified that the reduction in maternal phenotype was normalized in EDC-exposed pups raised by unexposed dams, but no reversal of the pubertal phenotype was achieved. DISCUSSION: Rats developmentally exposed to an EDC mixture exhibited multi- and transgenerational disruption of sexual maturation and maternal care via hypothalamic epigenetic reprogramming. These results raise concerns about the impact of EDC mixtures on future generations. [ABSTRACT FROM AUTHOR]
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- 2021
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5. Evidence for a long-term protection of wheel-running exercise against cocaine psychomotor sensitization in adolescent but not in adult mice.
- Author
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Lespine, Louis-Ferdinand and Tirelli, Ezio
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RODENTS , *LOCAL anesthetics , *COCAINE , *ADOLESCENT analysis , *ADOLESCENT psychotherapy - Abstract
Rodents housed with a running wheel can exhibit attenuated cocaine seeking and cocaine-induced psychomotor activation. However, the longevity of such a protection and the influence of the developmental stage during which exercise is displayed received little attention. Here, females and males C57BL/6J mice, aged 28 (adolescents) or 77 (adults) days were housed with (n = 56) or without (n = 28) a running wheel. After 3 weeks in these conditions, half of the exercised mice were deprived of their wheel (n = 28) whereas the other half and the sedentary mice were kept in their respective environments. After 3 additional weeks, mice were tested for initiation of psychomotor sensitization to 9 once-daily intraperitoneal injections of 8 mg/kg cocaine (following 2 drug-free sessions). The expression of sensitization was assessed on a single session 30 days after the last cocaine injection. Continuously exercised mice (wheel throughout experimentation) were less responsive to the initiation and the expression of cocaine effects, regardless of the gender and the developmental period during which exercise was introduced. A 3-week regimen of wheel-running exercise during adolescence (from 28 to 50 days of age) attenuated in later life the initiation and the expression of sensitization in females and its expression in males. In contrast, females and males previously exercised as adults (from 77 to 99 days of age) and their corresponding sedentary counterparts exhibited indiscernible levels of initiation and expression of sensitization. These results suggest that early-life period such as adolescence may be particularly sensitive to the long-term protection of exercise against cocaine vulnerability. [ABSTRACT FROM AUTHOR]
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- 2018
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6. Ontogenesis of behavioral sensitization and conditioned place preference induced by psychostimulants in laboratory rodents
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Tirelli, Ezio, Laviola, Giovanni, and Adriani, Walter
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BRAIN , *ONTOGENY , *NEWBORN infants - Abstract
The present review deals mainly with the ontogenesis of two important phenomena involved in vulnerability to several neuropsychiatric disorders, namely with drug-induced sensitization (both contextual and non-contextual) and with conditioned place preference. The term ‘infancy’ covers the first three postnatal weeks during development in rats and mice. Conversely, the term ‘adolescence’ may cover the whole postnatal period ranging from weaning (PND 21) to adulthood (at least PND 60) or specifically the period around the onset of puberty (animals aged 33–44 days). Recent studies in rats demonstrated that the establishment of a context-dependent sensitization appears during the first (for repeated drug administration) or during the second (for a single drug administration) postnatal week. However, the memory of drug-context association is transient in developing pups (lasting one or two days following the drug pretreatment). The long-term retention of drug-context associations matures progressively, and is complete by the third week of postnatal life. Finally, those mechanisms responsible for an adult-like profile of context-independent pharmacological sensitization appear later during ontogenesis, being mature by the fourth week of postnatal life. Another set of experiments extended this ontogenetic characterization by comparing adolescent and adult mice. When compared to the latter, the former subjects exhibit a greater amphetamine-induced locomotor sensitization, almost no sensitization of aversive stereotyped behaviors, and a less marked place conditioning. The strength of the drug-induced place conditioning was also directly compared with the unconditioned novelty-seeking drive. In conclusion, neonatal rats are able to show a relatively short-lasting retention of sensitized drug effects (short-term sensitization), whereas the ability to exhibit relatively long-lasting sensitized effects matures progressively during infancy (long-term sensitization). On the other hand, adolescent mice show a reduced sensitization of drug-induced psychotic symptoms, together with a more marked sensitization of arousing and euphorigenic properties of the drug and a reduced incentive memory of its hedonic effects. These age-related changes do imply very different degrees of vulnerability to drug addiction and several other neuropsychiatric disorders. [Copyright &y& Elsevier]
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- 2003
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7. Chronic tolerance to ethanol-induced sedation: Implication for age-related differences in locomotor sensitization.
- Author
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Quoilin, Caroline, Didone, Vincent, Tirelli, Ezio, and Quertemont, Etienne
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ETHANOL , *MUSCULOSKELETAL system physiology , *AGE factors in brain function localization , *CONSCIOUS sedation , *ALCOHOLISM , *BIOCOMPATIBILITY , *LABORATORY mice , *PHYSIOLOGY - Abstract
The adolescent brain has been suggested to be particularly sensitive to ethanol-induced neuroadaptations, which in turn could increase the risk of youths for alcohol abuse and dependence. Sensitization to the locomotor stimulant effects of ethanol has often been used as an animal model of ethanol-induced neuroadaptations. Previously, we showed that young mice were more sensitive than adults to the locomotor sensitization induced by high ethanol doses. However, this effect could be due to age-related differences in chronic tolerance to the sedative effects of ethanol. The aim of the present study is to assess chronic tolerance to the sedative effects of ethanol in weaning 21-day-old (P21), adolescent 35-day-old (P35) and adult 63-day-old (P63) female Swiss mice. After a daily injection of saline or 4 g/kg ethanol during 6 consecutive days, all P21, P35 and P63 mice were injected with 4 g/kg ethanol and submitted to the loss of righting reflex procedure. Our results confirm that the sensitivity to the acute sedative effects of ethanol gradually increases with age. Although this schedule of ethanol injections induces significant age-related differences in ethanol sensitization, it did not reveal significant differences between P21, P35 and P63 mice in the development of a chronic ethanol tolerance to its sedative effects. The present results show that age-related differences in the development of ethanol sensitization cannot be explained by differences in chronic ethanol tolerance to its sedative effects. More broadly, they do not support the idea that ethanolinduced sensitization is a by-product of chronic ethanol tolerance. [ABSTRACT FROM AUTHOR]
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- 2013
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8. Chronic ethanol exposure during adolescence alters the behavioral responsiveness to ethanol in adult mice
- Author
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Quoilin, Caroline, Didone, Vincent, Tirelli, Ezio, and Quertemont, Etienne
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UNDERAGE drinking , *ETHANOL , *ALCOHOL-induced disorders , *BEHAVIORAL assessment of teenagers , *SEDATIVES , *ALCOHOL drinking , *LABORATORY mice - Abstract
Abstract: Alcohol exposure during early adolescence is believed to durably alter the behavioral properties of ethanol, increasing the likelihood of later alcohol-related disorders. The aim of the present experiments was to characterize changes in the behavioral effects of ethanol in adult female Swiss mice after a chronic ethanol exposure during adolescence, extending from postnatal day 28 to postnatal day 42. After a chronic ethanol exposure during adolescence (daily injections of 0, 2.5 or 4g/kg ethanol for 14 consecutive days), adult mice were tested at postnatal day 63. The locomotor stimulant effects of ethanol, together with ethanol sensitization were tested in experiment 1. In experiment 2, the sedative effects of ethanol were assessed with the loss of righting reflex procedure. Finally, in experiment 3, the anxiolytic effects of ethanol were tested with the light/dark box test. Adult mice chronically exposed to ethanol during adolescence showed a lower basal locomotor activity, but higher locomotor stimulant effects of ethanol than non-exposed mice. Additionally, these adult mice developed higher rates of ethanol sensitization after chronic re-exposure to ethanol in adulthood. Adult mice exposed to ethanol during adolescence also had a stronger tolerance to the sedative effects of high ethanol doses, although they showed no evidence of changes in the anxiolytic effects of ethanol. These results are in agreement with the thesis that chronic alcohol consumption during adolescence, especially in high amounts, increases the risk of later alcohol-related disorders. [Copyright &y& Elsevier]
- Published
- 2012
- Full Text
- View/download PDF
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