Cognitive effects of early life exposure to PCBs: Sex-specific behavioral, hormonal and neuromolecular mechanisms involving the brain dopamine system.

Emily N Hilz, Cameron Schnurer, Swati Bhamidipati, Jahnabi Deka, Lindsay M Thompson, Andrea C Gore
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Abstract

Endocrine-disrupting chemicals (EDCs) are environmental toxicants that disrupt hormonal and neurodevelopmental processes. Among these chemicals, polychlorinated biphenyls (PCBs) are particularly concerning due to their resistance to biodegradation and tendency to bioaccumulate. PCBs affect neurodevelopmental function and disrupt the brain's dopamine (DA) system, which is crucial for attentional, affective, and reward processing. These disruptions may contribute to the rising prevalence of DA-mediated neuropsychiatric disorders such as ADHD, depression, and substance use disorders. Notably, these behaviors are sexually dimorphic, in part due to differences in sex hormones and their receptors, which are targets of estrogenic PCBs. Therefore, this study determined effects of early life PCB exposure on behaviors and neurochemistry related to potential disruption of dopaminergic signaling. Male and female Sprague Dawley rats were exposed to PCBs or vehicle perinatally and then underwent a series of behavioral tests, including the sucrose preference test to measure affect, conditioned orienting to assess incentive-motivational phenotype, and attentional set-shifting to evaluate cognitive flexibility and response latency. Following these tests, rats were euthanized, and we measured serum estradiol (E2), midbrain DA cells, and gene expression in the midbrain. Female rats exposed perinatally to A1221 exhibited decreased sucrose preference, and both male and female A1221 rats had reduced response latency in the attentional set-shifting task compared to vehicle counterparts. Conditioned orienting, serum estradiol (E2), and midbrain DA cell numbers were not affected in either sex; however, A1221-exposed male rats displayed higher expression of estrogen receptor alpha (Esr1) in the midbrain and non-significant effects on other DA-signaling genes. Additionally, E2 uniquely predicted behavioral outcomes and DAergic cell numbers in A1221-exposed female rats, whereas DA signaling genes were predictive of behavioral outcomes in males. These data highlight sex-specific effects of A1221 on neuromolecular and behavioral phenotypes.
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早期接触多氯联苯对认知的影响:涉及大脑多巴胺系统的性别特异性行为、荷尔蒙和神经分子机制。
干扰内分泌的化学品 (EDC) 是一种破坏荷尔蒙和神经发育过程的环境毒物。在这些化学品中,多氯联苯(PCBs)尤其令人担忧,因为它们不易被生物降解,而且容易生物累积。多氯联苯会影响神经发育功能,破坏大脑的多巴胺(DA)系统,而该系统对于注意力、情感和奖赏处理至关重要。这些干扰可能是导致多巴胺介导的神经精神疾病(如多动症、抑郁症和药物使用障碍)发病率上升的原因。值得注意的是,这些行为具有性别二态性,部分原因是性激素及其受体的差异,而这些受体是雌激素多氯联苯的靶标。因此,本研究确定了早期接触多氯联苯对行为和神经化学的影响,这些行为和神经化学与多巴胺能信号传递的潜在干扰有关。雄性和雌性 Sprague Dawley 大鼠在围产期暴露于多氯联苯或载体,然后接受一系列行为测试,包括测量情感的蔗糖偏好测试、评估激励-动机表型的条件定向,以及评估认知灵活性和反应潜伏期的注意集转移。这些测试结束后,大鼠被安乐死,我们测量了血清雌二醇(E2)、中脑DA细胞和中脑基因表达。围产期暴露于A1221的雌性大鼠表现出对蔗糖的偏好降低,与车辆大鼠相比,雄性和雌性A1221大鼠在注意集合转移任务中的反应潜伏期都缩短了。雌雄大鼠的条件定向、血清雌二醇(E2)和中脑DA细胞数量均未受到影响;然而,暴露于A1221的雄性大鼠中脑雌激素受体α(Esr1)的表达较高,且对其他DA信号基因无显著影响。此外,E2 对暴露于 A1221 的雌性大鼠的行为结果和 DA 能细胞数量具有独特的预测作用,而 DA 信号转导基因对雄性大鼠的行为结果具有预测作用。这些数据突显了A1221对神经分子和行为表型的性别特异性影响。
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