2006
DOI: 10.1111/j.1365-2605.2005.00563.x
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Disruption of reproductive development in male rat offspring following in utero exposure to phthalate esters

Abstract: Certain Phthalate esters have been shown to produce reproductive toxicity in male rodents with an age dependent sensitivity in effects with foetal animals being more sensitive than neonates which are in turn more sensitive than pubertal and adult animals. While the testicular effects of phthalates in rats have been known for more than 30 years, recent attention has been focused on the ability of these agents to produce effects on reproductive development in male offspring after in utero exposure. These esters … Show more

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Cited by 518 publications
(358 citation statements)
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“…For example, in male rats exposed to phthalates in utero, reduced anogenital distance, nipple retention and agenesis of the Wolffian ducts are consistently observed [14,15]. While these effects do not occur with 100% frequency, their dependence on androgens supports the suggestion that phthalates cause anti-androgenic effects in vivo.…”
Section: Plasma Hormone Concentrations Spiggin Concentrations and Rmentioning
confidence: 77%
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“…For example, in male rats exposed to phthalates in utero, reduced anogenital distance, nipple retention and agenesis of the Wolffian ducts are consistently observed [14,15]. While these effects do not occur with 100% frequency, their dependence on androgens supports the suggestion that phthalates cause anti-androgenic effects in vivo.…”
Section: Plasma Hormone Concentrations Spiggin Concentrations and Rmentioning
confidence: 77%
“…However, the discovery that some phthalates were weakly estrogenic in vitro [13] led to an intense period of study of phthalates as potential endocrine disruptors. After much research, it is now firmly established that di-ethylhexyl phthalate (DEHP), DBP, benzyl-butyl phthalate (BBP), diiso-butyl phthalate, di-iso-nonyl phthalate, di-hexyl phthalate, and di-pentyl phthalate are anti-androgenic endocrine disrupters in mammals [14,15]. However, it appears that they do not act directly as androgen receptor antagonists, or interfere with the genetic expression of the androgen receptor [14,16].…”
Section: Introductionmentioning
confidence: 99%
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“…In mammals, including humans, phthalate exposure is associated with endocrine disruption [15][16][17] and metabolic disorders [18,19]. In rodents, in utero exposure to phthalates results in developmental and reproductive defects similar to those termed testicular dysgenesis syndrome in humans [20][21][22].…”
Section: Introductionmentioning
confidence: 99%
“…Ils sont trĂšs rĂ©pandus dans l'environnement et l'on peut Ă©galement les trouver dans les aliments, aprĂšs leur migration Ă  partir d'emballages. Le phtalate de di-n-butyle, le phtalate de butylbenzyle et le phtalate de di-(2-Ă©thylhexyle) peuvent provoquer, via une action anti-androgĂ©nique, une atteinte de l'appareil reproducteur mĂąle (au cours du dĂ©veloppe-ment et au stade adulte) et une toxicitĂ© embryo-foetale pouvant conduire Ă  une augmentation de la mortalitĂ© intra-utĂ©rine ou Ă  une diminution du taux de survie postnatale [22,23]. En se liant au rĂ©cepteur des androgĂšnes, les phtalates bloquent le fonctionnement normal de ces hormones, sans pour autant activer ces rĂ©cepteurs (effet antagoniste).…”
Section: Phtalatesunclassified