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邻苯二甲酸二丁酯暴露导致 Wistar 大鼠神经递质系统的调制:多代评估。

Exposure to Di-n-butyl Phthalate Causes Modulation in Neurotransmitter System of Wistar Rats: A Multigenerational Assessment.

机构信息

Department of Biotechnology and Genetics, M S Ramaiah College of Arts, Science and Commerce, Bangalore, India.

Department of Zoology, Bangalore University, Bangalore, India.

出版信息

Int J Toxicol. 2024 Dec;43(6):579-589. doi: 10.1177/10915818241278670. Epub 2024 Sep 12.

Abstract

Neuroendocrine regulation is disrupted by di-n-butyl phthalate (DBP) when exposure occurs during the critical periods of fetal development, which can lead to neurological disorders. To evaluate the toxic potential of DBP, it is necessary to conduct teratological studies, which could determine impacts on the development of the fetus. The present study was designed to understand the sequelae of neuroendocrine regulation in one-month-old pups when rats were exposed to DBP (F-F) and during lactation. The rats received DBP (500 mg/kg BW/day) dissolved in olive oil through oral gavage from gestation day 6 to postnatal day 30, while the control group received the olive oil (vehicle) during the same timeline. Following the exposure, thyroid profile and estradiol, which were measured at GD-19, exhibited a significant decrease ( < 0.05) in dams (F-F). The exposure resulted in developmental outcomes, including underdeveloped fetuses, and a notable number of resorptions in experimental rats. The one-month-old pups were assessed for serum thyroid profile and testosterone and neurotransmitters in discrete brain regions, cerebral cortex, cerebellum, and hippocampus for up to three generations. The levels of dopamine and cortisol showed a significant increase ( < 0.05), but serotonin levels decreased when examined in distinct brain regions of the experimental group as compared to the control. DBP, which is considered an endocrine disruptor, had the most impact on the third generation in this study, leading to a significant decrease in testosterone levels. In summary, exposure to DBP impaired the neuroendocrine system and had an antiandrogenic effect in the three successive generations.

摘要

神经内分泌调节会被邻苯二甲酸二丁酯(DBP)破坏,如果在胎儿发育的关键时期暴露于 DBP 中,可能会导致神经紊乱。为了评估 DBP 的毒性潜力,有必要进行致畸研究,这可以确定其对胎儿发育的影响。本研究旨在了解大鼠在妊娠第 6 天至产后第 30 天经口灌胃接受 DBP(F-F)和哺乳期暴露时 1 个月大幼崽的神经内分泌调节后遗症。对照组在同一时间内接受橄榄油(载体)。暴露后,甲状腺图谱和雌二醇(在 GD-19 测量)在 F-F 母鼠中显著降低(<0.05)。暴露导致了发育结果,包括胎儿发育不全和实验大鼠中明显的吸收。对 1 个月大的幼崽进行了血清甲状腺图谱和睾丸激素以及离散脑区(大脑皮层、小脑和海马体)中的神经递质的评估,最多进行了三代。与对照组相比,实验组不同脑区的多巴胺和皮质醇水平显著升高(<0.05),而血清素水平降低。DBP 被认为是一种内分泌干扰物,在本研究中对第三代的影响最大,导致睾丸激素水平显著降低。总之,DBP 暴露破坏了神经内分泌系统,并在连续三代中具有抗雄激素作用。

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