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性激素结合球蛋白在体外和体内向神经元及脑细胞的内化。

Internalization of sex hormone-binding globulin into neurons and brain cells in vitro and in vivo.

作者信息

Caldwell J D, Shapiro R A, Jirikowski G F, Suleman F

机构信息

Department of Biomedical Sciences, University of Illinois College of Medicine, Rockford, IL, USA.

出版信息

Neuroendocrinology. 2007;86(2):84-93. doi: 10.1159/000107072. Epub 2007 Aug 6.

Abstract

BACKGROUND

Sex hormone-binding globulin (SHBG) is a 94-kDa homodimer that binds steroids and is made in the hypothalamus. We have demonstrated that infusions of SHBG into the hypothalami of rats increase their female sexual receptivity except when SHBG is coupled to dihydrotestosterone (DHT) suggesting that SHBG has an active function in behavioral neuroendocrinology.

METHODS

This study examines the possibility that SHBG is internalized by neuronal and/or non-neuronal brain cells as one possible mode of action using in vitro and in vivo techniques.

RESULTS

First, analysis of the uptake of radiolabeled SHBG ((125)I-SHBG) found (125)I-SHBG uptake in HT22 hippocampal cells stably transfected with cDNA for ER beta (HT22-ER beta). The addition of DHT to (125)I-SHBG significantly inhibited (125)I-SHBG uptake in HT22-ER beta cells but not in HT22-ER alpha or HT22 wild-type cells. SHBG internalization was specific as it did not occur in either the human neuroblastoma cell line SK-N-SH or the glioma cell line C6. Second, SHBG was labeled with a fluor (Alexa-555), and infused into the lateral cerebroventricles of ovariectomized rats. Optimal SHBG uptake was seen 10 min after these infusions. SHBG uptake was seen in specific parts of the choroid plexus and periventricular cells as well as into cells in the paraventricular nucleus, the medial forebrain bundle, and the habenula.

CONCLUSIONS

These studies suggest that SHBG is internalized by brain cells, which may be affected by the presence of ER beta. The gonadal steroids have numerous effects in brain and the discovery that the steroid-binding protein SHBG is taken up into neurons and brain cells may demand a change in thinking about how steroids are delivered to brain cells to affect neurophysiology.

摘要

背景

性激素结合球蛋白(SHBG)是一种94千道尔顿的同二聚体,可结合类固醇,由下丘脑产生。我们已经证明,向大鼠下丘脑注射SHBG会增加其雌性性接受能力,但当SHBG与双氢睾酮(DHT)偶联时除外,这表明SHBG在行为神经内分泌学中具有活性功能。

方法

本研究使用体外和体内技术,探讨SHBG被神经元和/或非神经元脑细胞内化作为一种可能作用方式的可能性。

结果

首先,对放射性标记的SHBG((125)I-SHBG)摄取的分析发现,在稳定转染了ERβ cDNA的HT22海马细胞(HT22-ERβ)中有(125)I-SHBG摄取。向(125)I-SHBG中添加DHT可显著抑制HT22-ERβ细胞中(125)I-SHBG的摄取,但对HT22-ERα或HT22野生型细胞无此作用。SHBG的内化具有特异性,因为在人神经母细胞瘤细胞系SK-N-SH或胶质瘤细胞系C6中均未发生。其次,用荧光染料(Alexa-555)标记SHBG,并注入去卵巢大鼠的侧脑室。注射后10分钟可见最佳的SHBG摄取。在脉络丛和室周细胞的特定部位以及室旁核、内侧前脑束和缰核的细胞中可见SHBG摄取。

结论

这些研究表明SHBG被脑细胞内化,这可能受ERβ的存在影响。性腺类固醇在大脑中有多种作用,类固醇结合蛋白SHBG被神经元和脑细胞摄取这一发现可能需要改变我们对类固醇如何传递到脑细胞以影响神经生理学的认识。

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