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雌激素诱导发育中的浦肯野细胞树突生长、棘突形成和突触形成的作用方式及功能意义。

Mode of action and functional significance of estrogen-inducing dendritic growth, spinogenesis, and synaptogenesis in the developing Purkinje cell.

作者信息

Sasahara Katsunori, Shikimi Hanako, Haraguchi Shogo, Sakamoto Hirotaka, Honda Shin-ichiro, Harada Nobuhiro, Tsutsui Kazuyoshi

机构信息

Laboratory of Brain Science, Faculty of Integrated Arts and Sciences, Hiroshima University, Higashi-Hiroshima 739-8521, Japan.

出版信息

J Neurosci. 2007 Jul 11;27(28):7408-17. doi: 10.1523/JNEUROSCI.0710-07.2007.

Abstract

Neurosteroids are synthesized de novo from cholesterol in the brain. To understand neurosteroid action in the brain, data on the regio- and temporal-specific synthesis of neurosteroids are needed. Recently, we identified the Purkinje cell as an active neurosteroidogenic cell. In rodents, this neuron actively produces several neurosteroids including estradiol during neonatal life, when cerebellar neuronal circuit formation occurs. Estradiol may be involved in cerebellar neuronal circuit formation through promoting neuronal growth and neuronal synaptic contact, because the Purkinje cell expresses estrogen receptor-beta (ERbeta). To test this hypothesis, in this study we examined the effects of estradiol on dendritic growth, spinogenesis, and synaptogenesis in the Purkinje cell using neonatal wild-type (WT) mice or cytochrome P450 aromatase knock-out (ArKO) mice. Administration of estradiol to neonatal WT or ArKO mice increased dendritic growth, spinogenesis, and synaptogenesis in the Purkinje cell. In contrast, WT mice treated with tamoxifen, an ER antagonist, or ArKO mice exhibited decreased Purkinje dendritic growth, spinogenesis, and synaptogenesis at the same neonatal period. To elucidate the mode of action of estradiol, we further examined the expression of brain-derived neurotrophic factor (BDNF) in response to estrogen actions in the neonate. Estrogen administration to neonatal WT or ArKO mice increased the BDNF level in the cerebellum, whereas tamoxifen decreased the BDNF level in WT mice similar to ArKO mice. BDNF administration to tamoxifen-treated WT mice increased Purkinje dendritic growth. These results indicate that estradiol induces dendritic growth, spinogenesis, and synaptogenesis in the developing Purkinje cell via BDNF action during neonatal life.

摘要

神经甾体在大脑中由胆固醇从头合成。为了解神经甾体在大脑中的作用,需要有关神经甾体区域和时间特异性合成的数据。最近,我们确定浦肯野细胞是一种活跃的神经甾体生成细胞。在啮齿动物中,当小脑神经元回路形成时,这种神经元在新生期会活跃地产生几种神经甾体,包括雌二醇。由于浦肯野细胞表达雌激素受体β(ERβ),雌二醇可能通过促进神经元生长和神经元突触接触参与小脑神经元回路的形成。为了验证这一假设,在本研究中,我们使用新生野生型(WT)小鼠或细胞色素P450芳香化酶基因敲除(ArKO)小鼠,研究了雌二醇对浦肯野细胞树突生长、棘突形成和突触形成的影响。给新生WT或ArKO小鼠注射雌二醇可增加浦肯野细胞的树突生长、棘突形成和突触形成。相比之下,在同一新生期,用雌激素拮抗剂他莫昔芬处理的WT小鼠或ArKO小鼠的浦肯野树突生长、棘突形成和突触形成减少。为了阐明雌二醇的作用模式,我们进一步研究了新生儿雌激素作用后脑源性神经营养因子(BDNF)的表达。给新生WT或ArKO小鼠注射雌激素可提高小脑中BDNF水平,而他莫昔芬可降低WT小鼠的BDNF水平,类似于ArKO小鼠。给他莫昔芬处理的WT小鼠注射BDNF可增加浦肯野树突的生长。这些结果表明,在新生期,雌二醇通过BDNF作用诱导发育中的浦肯野细胞的树突生长、棘突形成和突触形成。

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