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κ-阿片受体表达定义了星形胶质细胞的一个表型独特的亚群:与Ca2+动员、发育以及阿片类药物的抗增殖作用的关系。

kappa-opioid receptor expression defines a phenotypically distinct subpopulation of astroglia: relationship to Ca2+ mobilization, development, and the antiproliferative effect of opioids.

作者信息

Gurwell J A, Duncan M J, Maderspach K, Stiene-Martin A, Elde R P, Hauser K F

机构信息

Department of Anatomy and Neurobiology, University of Kentucky Medical Center, Lexington, KY 40536-0084, USA.

出版信息

Brain Res. 1996 Oct 21;737(1-2):175-87. doi: 10.1016/0006-8993(96)00728-7.

Abstract

To assess the role of kappa-opioid receptors in astrocyte development, the effect of kappa-agonists on the growth of astroglia derived from 1-2-day-old mouse cerebra was examined in vitro. kappa-Opioid receptor expression was assessed immunocytochemically (using KA8 and KOR1 antibodies), as well as functionally by examining the effect of kappa-receptor activation on intracellular calcium ([Ca2+]i) homeostasis and DNA synthesis. On days 6-7, as many as 50% of the astrocytes displayed kappa-receptor (KA8) immunoreactivity or exhibited increases in [Ca2+]i in response to kappa-agonist treatment (U69,593 or U50,488H). Exposure to U69,593 (100 nM) for 72 h caused a significant reduction in number and proportion of glial fibrillary acidic protein-immunoreactive astrocytes incorporating bromodeoxyuridine (BrdU) that could be prevented by co-administering the kappa-antagonist, nor-binaltorphimine (300 nM). In contrast, on day 14, only 5 or 14%, respectively, of the astrocytes were kappa-opioid receptor (KA8) immunoreactive or displayed functional increases in [Ca2+]i. Furthermore, U69,593 (100 nM) treatment failed to inhibit BrdU incorporation at 9 days in vitro. Experimental manipulations showed that kappa-receptor activation increases astroglial [Ca2+]i both through influx via L-type channels and through mobilization of intracellular stores (which is an important Ca2+ signaling pathway in cell division). Collectively, these results indicate that a subpopulation of developing astrocytes express kappa-opioid receptors in vitro, and suggest that the activation of kappa-receptors mobilizes [Ca2+]i and inhibits cell proliferation. Moreover, the proportion of astrocytes expressing kappa-receptors was greatest during a period of rapid cell growth suggesting that they are preferentially expressed by proliferating astrocytes.

摘要

为评估κ-阿片受体在星形胶质细胞发育中的作用,在体外研究了κ-激动剂对源自1-2日龄小鼠大脑的星形胶质细胞生长的影响。采用免疫细胞化学方法(使用KA8和KOR1抗体)评估κ-阿片受体的表达,并通过检测κ-受体激活对细胞内钙([Ca2+]i)稳态和DNA合成的影响来进行功能评估。在第6-7天,多达50%的星形胶质细胞显示κ-受体(KA8)免疫反应性,或在κ-激动剂处理(U69,593或U50,488H)后表现出[Ca2+]i增加。暴露于U69,593(100 nM)72小时导致掺入溴脱氧尿苷(BrdU)的胶质纤维酸性蛋白免疫反应性星形胶质细胞的数量和比例显著减少,而共同给予κ-拮抗剂 nor-binaltorphimine(300 nM)可预防这种情况。相比之下,在第14天,分别只有5%或14%的星形胶质细胞具有κ-阿片受体(KA8)免疫反应性或表现出功能性[Ca2+]i增加。此外,U69,593(100 nM)处理在体外培养9天时未能抑制BrdU掺入。实验操作表明,κ-受体激活通过L型通道内流和细胞内储存的动员增加星形胶质细胞的[Ca2+]i(这是细胞分裂中重要的Ca2+信号通路)。总体而言,这些结果表明,发育中的星形胶质细胞亚群在体外表达κ-阿片受体,并提示κ-受体的激活可动员[Ca2+]i并抑制细胞增殖。此外,在细胞快速生长期间,表达κ-受体的星形胶质细胞比例最大,这表明它们优先由增殖的星形胶质细胞表达。

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