首页> 美国卫生研究院文献>European Journal of Histochemistry : EJH >Aromatase immunoreactivity in fetal ovine neuronal cell cultures exposed to oxidative injury
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Aromatase immunoreactivity in fetal ovine neuronal cell cultures exposed to oxidative injury

机译:暴露于氧化损伤的胎儿绵羊神经元细胞培养物中的芳香化酶免疫反应性

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摘要

A lot of evidence testifies that aromatase is expressed in the central nervous system where it has been detected not only in hypothalamic and limbic regions but also in the cerebral cortex and spinal cord. In physiological conditions, aromatase is expressed exclusively by neurons, where it has been mainly found in cell bodies, processes and synaptic terminals. Moreover, primary cultured cortical astrocytes from female rats are more resistant to oxidant cell death than those from males, suggesting a protective role of estradiol. The aim of this study was to evaluate changes in aromatase expression in response to 3-nitro-L-tyrosine, a marker of oxidative stress, in primary neuronal cell cultures from brains of 60-day old sheep fetuses. Cells were identified as neurons by using class III β-tubulin, a marker of neuronal cells. Two morphological types were consistently recognizable: i) bipolar cells with an oval cell body; ii) multipolar cells whose processes formed a wide net with those of adjacent cells. In situ hybridization technique performed on 60-day old fetal neurons revealed that in baseline conditions aromatase gene expression occurs. Importantly, cells exposed to 360 µM 3-nitro-L-tyrosine were fewer and showed more globular shape and shorter cytoplasmic processes in comparison to control cells. The immunocytochemical study with anti-aromatase antibody revealed that cells exposed to 360 µM 3-nitro-L-tyrosine were significantly more immunoreactive than control cells. Thus, it can be postulated that the oxidant effects of the amino acid analogue 3-nitro-L-tyrosine could be counterbalanced by an increase in aromatase expression that in turn can lead to the formation of neuroprotective estradiol via aromatization of testosterone.
机译:许多证据证明,芳香酶在中枢神经系统中表达,不仅在下丘脑和边缘区域而且在大脑皮层和脊髓中都检测到。在生理条件下,芳香化酶仅由神经元表达,主要在细胞体,过程和突触末端中发现。此外,雌性大鼠的原代培养皮质星形胶质细胞比雄性大鼠的皮质星形胶质细胞对氧化剂细胞的死亡更有抵抗力,表明雌二醇具有保护作用。这项研究的目的是评估60天大的绵羊胎儿大脑中原始神经元细胞培养物中对氧化应激标记物3-硝基-L-酪氨酸的响应。通过使用III类β-微管蛋白(神经元细胞的标志物)将细胞鉴定为神经元。两种形态学类型是一致可识别的:i)具有卵形细胞体的双极细胞; ii)多极细胞,其过程与相邻细胞的过程形成一个宽网。在60天大的胎儿神经元上进行的原位杂交技术表明,在基线条件下会出现芳香化酶基因表达。重要的是,与对照细胞相比,暴露于360 µM 3-硝基-L-酪氨酸的细胞更少,显示出更多的球状形状和较短的细胞质过程。用抗芳香化酶抗体进行的免疫细胞化学研究表明,暴露于360 µM 3-硝基-L-酪氨酸的细胞的免疫反应性明显高于对照细胞。因此,可以推测,氨基酸类似物3-硝基-L-酪氨酸的氧化作用可以通过芳香化酶表达的增加而抵消,芳香化酶表达的增加反过来又可以导致睾丸激素芳香化形成神经保护性雌二醇。

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