Department of Psychiatry and Behavioral Sciences, Duke University School of Medicine, Durham, NC, USA.
Nicholas School of the Environment, Duke University, Durham, NC, USA.
Neurotoxicol Teratol. 2022 Sep-Oct;93:107121. doi: 10.1016/j.ntt.2022.107121. Epub 2022 Sep 9.
Polycyclic aromatic hydrocarbons (PAH) are products of incomplete combustion which are ubiquitous pollutants and constituents of harmful mixtures such as tobacco smoke, petroleum and creosote. Animal studies have shown that these compounds exert developmental toxicity in multiple organ systems, including the nervous system. The relative persistence of or recovery from these effects across the lifespan remain poorly characterized. These studies tested for persistence of neurobehavioral effects in AB* zebrafish exposed 5-120 h post-fertilization to a typical PAH, benzo[a]pyrene (BAP). Study 1 evaluated the neurobehavioral effects of a wide concentration range of BAP (0.02-10 μM) exposures from 5 to 120 hpf during larval (6 days) and adult (6 months) stages of development, while study 2 evaluated neurobehavioral effects of BAP (0.3-3 μM) from 5 to 120 hpf across four stages of development: larval (6 days), adolescence (2.5 months), adulthood (8 months) and late adulthood (14 months). Embryonic BAP exposure caused minimal effects on larval motility, but did cause neurobehavioral changes at later points in life. Embryonic BAP exposure led to nonmonotonic effects on adolescent activity (0.3 μM hyperactive, Study 2), which attenuated with age, as well as startle responses (0.2 μM enhanced, Study 1) at 6 months of age. Similar startle changes were also detected in Study 2 (1.0 μM), though it was observed that the phenotype shifted from reduced pretap activity to enhanced posttap activity from 8 to 14 months of age. Changes in the avoidance (0.02-10 μM, Study 1) and approach (reduced, 0.3 μM, Study 2) of aversive/social cues were also detected, with the latter attenuating from 8 to 14 months of age. Fish from study 2 were maintained into aging (18 months) and evaluated for overall and tissue-specific oxygen consumption to determine whether metabolic processes in the brain and other target organs show altered function in late life based on embryonic PAH toxicity. BAP reduced whole animal oxygen consumption, and overall reductions in total basal, mitochondrial basal, and mitochondrial maximum respiration in target organs, including the brain, liver and heart. The present data show that embryonic BAP exposure can lead to neurobehavioral impairment across the life-span, but that these long-term risks differentially emerge or attenuate as development progresses.
多环芳烃(PAH)是不完全燃烧的产物,是无处不在的污染物,也是烟草烟雾、石油和杂酚油等有害混合物的组成部分。动物研究表明,这些化合物会对多个器官系统产生发育毒性,包括神经系统。在整个生命周期中,这些影响的相对持久性或恢复情况仍未得到很好的描述。这些研究测试了 AB*斑马鱼在受精后 5-120 小时暴露于典型的多环芳烃苯并[a]芘(BAP)时的神经行为影响。研究 1 评估了从 5 至 120 hpf 期间在幼虫(6 天)和成年(6 个月)阶段暴露于广泛浓度范围的 BAP(0.02-10 μM)对神经行为的影响,而研究 2 评估了从 5 至 120 hpf 期间在四个发育阶段(幼虫(6 天)、青春期(2.5 个月)、成年(8 个月)和老年(14 个月))的 BAP(0.3-3 μM)的神经行为影响。胚胎 BAP 暴露对幼虫运动性的影响很小,但在生命后期会引起神经行为变化。胚胎 BAP 暴露会导致青春期活动的非单调影响(研究 2 中的 0.3 μM 表现出过度活跃),随着年龄的增长而减弱,以及在 6 个月大时的惊跳反应(研究 1 中的 0.2 μM 增强)。研究 2 也检测到类似的惊跳变化(1.0 μM),尽管观察到表型从 8 至 14 个月龄时的预触活动减少转变为后触活动增强。也检测到对回避(0.02-10 μM,研究 1)和接近(减少,0.3 μM,研究 2)的厌恶/社交线索的变化,后者从 8 至 14 个月龄时减弱。来自研究 2 的鱼被维持到衰老(18 个月)并评估整体和组织特异性耗氧量,以确定基于胚胎 PAH 毒性,大脑和其他靶器官中的代谢过程是否在晚年表现出功能改变。BAP 降低了动物的整体耗氧量,以及靶器官(包括大脑、肝脏和心脏)的总基础、线粒体基础和线粒体最大呼吸的整体降低。本数据表明,胚胎 BAP 暴露会导致整个生命周期的神经行为损伤,但这些长期风险会随着发育的进行而不同地出现或减弱。
