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神经甾体对海马树突棘的快速非基因组调节:雄激素、雌激素和皮质类固醇。

Rapid nongenomic modulation by neurosteroids of dendritic spines in the hippocampus: Androgen, oestrogen and corticosteroid.

机构信息

Department of Liberal Arts, Faculty of Medicine, Saitama Medical University, Iruma, Saitama, Japan.

Department of Biochemistry, Faculty of Medicine, Saitama Medical University, Iruma, Saitama, Japan.

出版信息

J Neuroendocrinol. 2018 Feb;30(2). doi: 10.1111/jne.12561.

Abstract

Memories are stored in synapses that consist of axon terminals and dendritic spines. Dendritic spines are postsynaptic structures of synapses and are essential for synaptic plasticity and cognition. Therefore, extensive investigations concerning the functions and structures of spines have been performed. Sex steroids and stress steroids have been shown to modulate hippocampal synapses. Although the rapid modulatory action of sex steroids on synapses has been studied in hippocampal neurones over several decades, the essential molecular mechanisms have not been fully understood. Here, a description of kinase-dependent signalling mechanisms is provided that can explain the rapid nongenomic modulation of dendritic spinogenesis in rat and mouse hippocampal slices by the application of sex steroids, including dihydrotestosterone, testosterone, oestradiol and progesterone. We also indicate the role of synaptic (classic) sex steroid receptors that trigger these rapid synaptic modulations. Moreover, we describe rapid nongenomic spine modulation by applying corticosterone, which is an acute stress model of the hippocampus. The explanations for the results obtained are mainly based on the optical imaging of dendritic spines. Comparisons are also performed with results obtained from other types of imaging, including electron microscopic imaging. Relationships between spine modulation and modulation of cognition are discussed. We recognise that most of rapid effects of exogenously applied oestrogen and androgen were observed in steroid-depleted conditions, including acute slices of the hippocampus, castrated male animals and ovariectomised female animals. Therefore, the previously observed effects can be considered as a type of recovery event, which may be essentially similar to hormone replacement therapy under hormone-decreased conditions. On the other hand, in gonadally intact young animals with high levels of endogenous sex hormones, further supplementation of sex hormones might not be effective, whereas the infusion of blockers for steroid receptors or kinases may be effective, with respect to suppressing sex hormone functions, thus providing useful information regarding molecular mechanisms.

摘要

记忆储存在由轴突末梢和树突棘组成的突触中。树突棘是突触的后突触结构,对于突触可塑性和认知至关重要。因此,已经进行了广泛的关于棘突的功能和结构的研究。性激素和应激激素已被证明可以调节海马突触。尽管几十年来一直在研究性激素对海马神经元突触的快速调节作用,但基本的分子机制尚未完全理解。在这里,提供了依赖激酶的信号转导机制的描述,该机制可以解释性激素(包括二氢睾酮、睾酮、雌二醇和孕酮)在大鼠和小鼠海马切片中对树突棘生成的快速非基因组调节。我们还指出了触发这些快速突触调节的突触(经典)性激素受体的作用。此外,我们描述了通过施加皮质酮(海马的急性应激模型)对快速非基因组棘突调节的作用。对获得的结果的解释主要基于树突棘的光学成像。还与包括电子显微镜成像在内的其他类型的成像结果进行了比较。讨论了棘突调节与认知调节之间的关系。我们认识到,在外源性雌激素和雄激素施加的大多数快速作用是在类固醇耗尽的条件下观察到的,包括海马的急性切片、去势雄性动物和去卵巢雌性动物。因此,先前观察到的作用可以被认为是一种恢复事件,其本质上可能与激素减少条件下的激素替代疗法相似。另一方面,在具有高水平内源性性激素的性腺完整的年轻动物中,进一步补充性激素可能无效,而类固醇受体或激酶的抑制剂的输注可能有效,从而抑制性激素的功能,从而提供关于分子机制的有用信息。

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