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首页> 外文期刊>Neuroendocrinology: International Journal for Basic and Clinical Studies on Neuroendocrine Relationships >Corticosteroids influence the action potential firing pattern of hippocampal subfield CA3 pyramidal cells.
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Corticosteroids influence the action potential firing pattern of hippocampal subfield CA3 pyramidal cells.

机译:皮质类固醇影响海马CA3区锥体细胞动作电位的发射模式。

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Corticosteroids regulate gene expression through the activation of mineralocorticoid and glucocorticoid receptors. The hippocampus contains the highest density of mineralocorticoid and glucocorticoid receptors in the central nervous system. The modulation of neuron excitability by corticosteroids in hippocampal subfield CA1 is well documented. However, it is not known whether corticosteroids produce different effects across the various hippocampal subfields. Therefore, we used intracellular recording techniques to examine the actions of chronic corticosteroid treatment (2 weeks) on the electrophysiological properties of rat hippocampal subfield CA3 pyramidal cells. The treatment groups used in this investigation were: adrenalectomy (ADX), selective mineralocorticoid receptor activation with aldosterone (ALD), mineralocorticoid and glucocorticoid receptor activation with high levels of corticosterone (HCT), and SHAM. Corticosteroid treatment altered the percentage of nonburst and burst firing neurons. The percentages of nonbursting cells were 74 and 62% in tissue from ADX and HCT animals compared to 42 and 41% in ALD and SHAM animals, respectively. The corticosteroid-induced effect on the ratio of nonbursting to bursting cells does not appear to be secondary to changes in the cell's membrane input resistance, resting potential, time constant, action potential, slow-or fast-afterhyperpolarizing potential properties. Based on these results we conclude that corticosteroids are important for maintaining the ratio of nonburst and burst firing pyramidal neurons in subfield CA3. These novel results are distinct from those previously reported for subfield CA1, suggesting that corticosteroids have different effects across hippocampal subfields.
机译:皮质类固醇通过盐皮质激素和糖皮质激素受体的激活来调节基因表达。海马在中枢神经系统中含有最高密度的盐皮质激素和糖皮质激素受体。皮质类固醇在海马亚区CA1中对神经元兴奋性的调节作用已得到充分证明。然而,尚不清楚皮质类固醇是否在各个海马亚区产生不同的作用。因此,我们使用细胞内记录技术来检查慢性皮质类固醇治疗(2周)对大鼠海马亚区CA3锥体细胞电生理特性的作用。本研究中使用的治疗组为:肾上腺切除术(ADX),醛固酮选择性激活盐皮质激素受体(ALD),高水平的皮质激素激活盐皮质激素和糖皮质激素受体(HCT)和SHAM。皮质类固醇激素治疗改变了非爆发和爆发性发射神经元的百分比。在ADX和HCT动物的组织中,非增生细胞的百分比分别为74%和62%,而ALD和SHAM动物分别为42%和41%。皮质类固醇诱导的对细胞不破裂与破裂的比率的影响似乎不是继发于细胞膜输入阻力,静息电位,时间常数,动作电位,慢极化或快极化后超极化电位特性变化的。根据这些结果,我们得出结论,皮质类固醇对于维持CA3子域中非爆发性和爆发性发射锥体神经元的比率很重要。这些新颖的结果与先前报道的子领域CA1的结果不同,表明皮质类固醇在海马子领域具有不同的作用。

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