Developmental exposure to methylmercury alters GAD67 immunoreactivity and morphology of endothelial cells and capillaries of midbrain and hindbrain regions of adult rat offspring

IF 2.6 3区 医学 Q3 NEUROSCIENCES Neurotoxicology and teratology Pub Date : 2024-01-01 DOI:10.1016/j.ntt.2024.107320
Nazneen Y. Rustom, James N Reynolds
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Abstract

Introduction

Methylmercury (MeHg) is an environmental contaminant that is of particular concern in Northern Arctic Canadian populations. Specifically, organic mercury compounds such as MeHg are potent toxicants that affect multiple bodily systems including the nervous system. Developmental exposure to MeHg is a major concern, as the developing fetus and neonate are thought to be especially vulnerable to the toxic effects of MeHg. The objective of this study was to examine developmental exposure to low doses of MeHg and effects upon the adult central nervous system (CNS). The doses of MeHg chosen were scaled to be proportional to the concentrations of MeHg that have been reported in human maternal blood samples in Northern Arctic Canadian populations.

Method

Offspring were exposed to MeHg maternally where pregnant Sprague Dawley rats were fed cookies that contained MeHg or vehicle (vehicle corn oil; MeHg 0.02 mg/kg/body weight or 2.0 mg/kg/body weight) daily, throughout gestation (21 days) and lactation (21 days). Offspring were not exposed to MeHg after the lactation period and were euthanized on postnatal day 450. Brains were extracted, fixed, frozen, and sectioned for immunohistochemical analysis. A battery of markers of brain structure and function were selected including neuronal GABAergic enzymatic marker glutamic acid decarboxylase-67 (GAD67), apoptotic/necrotic marker cleaved caspase-3 (CC3), catecholamine marker tyrosine hydroxylase (TH), immune inflammatory marker microglia (Cd11b), endothelial cell marker rat endothelial cell antigen-1 (RECA-1), doublecortin (DCX), Bergmann glia (glial fibrillary acidic protein (GFAP)), and general nucleic acid and cellular stains Hoechst, and cresyl violet, respectively. Oxidative stress marker lipofuscin (autofluorescence) was also assessed. Both male and female offspring were included in analysis. Two-way analysis of variance (ANOVA) was utilized where sex and treatment were considered as between-subject factors (p* <0.05). ImageJ was used to assess immunohistochemical results.

Results

In comparison with controls, adult rat offspring exposed to both doses of MeHg were observed to have (1) increased GAD67 in the cerebellum; (2) decreased lipofuscin in the locus coeruleus; and (3) decreased GAD67 in the anterior CA1 region. Furthermore, in the substantia nigra and periaqueductal gray, adult male offspring consistently had a larger endothelial cell and capillary perimeter in comparison to females. The maternal high dose of MeHg influenced RECA-1 immunoreactivity in both the substantia nigra and periaqueductal gray of adult rat offspring, where the latter neuronal region also showed statistically significant decreases in RECA-1 immunoreactivity at the maternal low dose exposure level. Lastly, males exposed to high doses of MeHg during development exhibited a statistically significant increase in the perimeter of endothelial cells and capillaries (RECA-1) in the cerebellum, in comparison to male controls.

Conclusion

Findings suggest that in utero and early postnatal exposure to MeHg at environmentally relevant doses leads to long-lasting and selective changes in the CNS. Exposure to MeHg at low doses may affect GABAergic homeostasis and vascular integrity of the CNS. Such changes may contribute to neurological disturbances in learning, cognition, and memory that have been reported in epidemiological studies.

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甲基汞的发育暴露会改变成年大鼠后代中脑和后脑区域内皮细胞和毛细血管的 GAD67 免疫活性和形态
导言甲基汞(MeHg)是一种环境污染物,在加拿大北极地区北部的人群中尤其令人担忧。具体来说,甲基汞等有机汞化合物是影响包括神经系统在内的多个身体系统的强效毒物。发育中的胎儿和新生儿特别容易受到甲基汞的毒性影响,因此,发育中接触甲基汞是一个主要问题。本研究的目的是研究发育期接触低剂量甲基汞对成人中枢神经系统(CNS)的影响。在整个妊娠期(21 天)和哺乳期(21 天),每天给怀孕的 Sprague Dawley 大鼠喂食含有甲基汞或载体(载体玉米油;甲基汞 0.02 毫克/千克/体重或 2.0 毫克/千克/体重)的饼干。后代在哺乳期后不再接触甲基汞,并在出生后第 450 天安乐死。提取、固定、冷冻和切片后进行免疫组化分析。选择了一系列大脑结构和功能的标记物,包括神经元 GABA 能酶标记物谷氨酸脱羧酶-67(GAD67)、凋亡/坏死标记物裂解的 Caspase-3 (CC3)、儿茶酚胺标记物酪氨酸羟化酶(TH)、免疫炎症标记物小胶质细胞(microglia)、神经元 GABA 能酶标记物谷氨酸脱羧酶-67(GAD67)、凋亡/坏死标记物裂解的 Caspase-3 (CC3)、儿茶酚胺标记物酪氨酸羟化酶(TH免疫炎症标记物小胶质细胞(Cd11b)、内皮细胞标记物大鼠内皮细胞抗原-1(RECA-1)、双皮质素(DCX)、伯格曼胶质细胞(胶质纤维酸性蛋白(GFAP)),以及一般核酸和细胞染色剂 Hoechst 和甲酚紫。此外,还对氧化应激标记脂褐质(自发荧光)进行了评估。雌雄后代均纳入分析。采用双向方差分析(ANOVA),将性别和处理视为受试者之间的因素(P* <0.05)。结果与对照组相比,暴露于两种剂量甲基汞的成年后代大鼠的(1)小脑中的GAD67增加;(2)脑室中的脂褐素减少;(3)CA1前区的GAD67减少。此外,在黑质和uctal周围灰质,成年雄性后代的内皮细胞和毛细血管周长一直大于雌性后代。母体高剂量甲基汞会影响成年后代黑质和视网膜周围灰质中的 RECA-1 免疫活性,而在母体低剂量暴露水平下,视网膜周围灰质中的 RECA-1 免疫活性也会出现统计学意义上的显著下降。最后,与雄性对照组相比,在发育过程中暴露于高剂量甲基汞的雄性大鼠小脑内皮细胞和毛细血管(RECA-1)的周长出现了统计学意义上的显著增加。低剂量接触甲基汞可能会影响 GABA 能平衡和中枢神经系统血管的完整性。流行病学研究报告称,这种变化可能会导致学习、认知和记忆方面的神经紊乱。
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来源期刊
CiteScore
5.60
自引率
10.30%
发文量
48
审稿时长
58 days
期刊介绍: Neurotoxicology and Teratology provides a forum for publishing new information regarding the effects of chemical and physical agents on the developing, adult or aging nervous system. In this context, the fields of neurotoxicology and teratology include studies of agent-induced alterations of nervous system function, with a focus on behavioral outcomes and their underlying physiological and neurochemical mechanisms. The Journal publishes original, peer-reviewed Research Reports of experimental, clinical, and epidemiological studies that address the neurotoxicity and/or functional teratology of pesticides, solvents, heavy metals, nanomaterials, organometals, industrial compounds, mixtures, drugs of abuse, pharmaceuticals, animal and plant toxins, atmospheric reaction products, and physical agents such as radiation and noise. These reports include traditional mammalian neurotoxicology experiments, human studies, studies using non-mammalian animal models, and mechanistic studies in vivo or in vitro. Special Issues, Reviews, Commentaries, Meeting Reports, and Symposium Papers provide timely updates on areas that have reached a critical point of synthesis, on aspects of a scientific field undergoing rapid change, or on areas that present special methodological or interpretive problems. Theoretical Articles address concepts and potential mechanisms underlying actions of agents of interest in the nervous system. The Journal also publishes Brief Communications that concisely describe a new method, technique, apparatus, or experimental result.
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