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亚砷酸盐暴露的小鼠不同脑区的砷形态、AS3MT 含量和 AS3MT 基因表达。

Arsenic species, AS3MT amount, and AS3MT gene expression in different brain regions of mouse exposed to arsenite.

机构信息

Departamento de Toxicología, CINVESTAV, México.

出版信息

Environ Res. 2010 Jul;110(5):428-34. doi: 10.1016/j.envres.2010.01.007.

Abstract

Human exposure to inorganic arsenic (iAs) has been associated with cancer and serious injury to various internal organs, as well as peripheral neuropathy, endocrine disruption and diverse effects in the central nervous system (CNS). Using rodent models, it is possible to demonstrate As accumulation in the brain that leads to defects in operant learning, behavioral changes, and affect pituitary gonadotrophins. iAs biomethylation in the CNS is a significant process, yielding products that are more reactive and toxic than the parent compound. Mice received 2.5, 5, and 10 mg/kg/day sodium arsenite orally for 9 days. We investigated the distribution of iAs and its metabolites as well as the mRNA and protein expression of arsenic (III) methyltransferase (AS3MT), which encodes the key enzyme in iAs metabolism, in the cerebral cortex, hippocampus, striatum, mesencephalon, thalamus, cerebellum, hypothalamus, pons, medulla oblongata, and pituitary of mouse brain. Our findings show that methylated As metabolites are present in all brain regions studied suggesting that AS3MT is ubiquitously expressed in the brain and it is not inducible by dose of arsenite. There is also a dose-related accumulation of As species in all brain regions, with the highest accumulation observed in the pituitary. The higher distribution of arsenicals in pituitary can help to explain the neuroendocrine effects associated with iAs exposure.

摘要

人类接触无机砷 (iAs) 已与癌症以及各种内部器官的严重损伤、周围神经病变、内分泌紊乱和中枢神经系统 (CNS) 的多种影响有关。使用啮齿动物模型,可以证明砷在大脑中的积累会导致操作性学习缺陷、行为改变以及影响垂体促性腺激素。CNS 中的 iAs 生物甲基化是一个重要的过程,产生的产物比母体化合物更具反应性和毒性。小鼠每天口服 2.5、5 和 10mg/kg 亚砷酸钠 9 天。我们研究了 iAs 及其代谢物的分布,以及编码 iAs 代谢关键酶的砷 (III) 甲基转移酶 (AS3MT) 的 mRNA 和蛋白质表达,在大脑皮层、海马体、纹状体、中脑、丘脑、小脑、下丘脑、脑桥、延髓和垂体。我们的研究结果表明,甲基化的 As 代谢物存在于所有研究的脑区,这表明 AS3MT 在大脑中广泛表达,并且不受亚砷酸钠剂量的诱导。所有脑区也存在与剂量相关的砷物种积累,其中在垂体中观察到的积累最高。砷剂在垂体中的更高分布有助于解释与 iAs 暴露相关的神经内分泌效应。

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