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脑神经元中儿茶酚胺分化所需的生长因子与递质之间的协同作用。

Synergy between growth factors and transmitters required for catecholamine differentiation in brain neurons.

作者信息

Du X, Iacovitti L

机构信息

Department of Neurology, Hahnemann University, Philadelphia, Pennsylvania 19102, USA.

出版信息

J Neurosci. 1995 Jul;15(7 Pt 2):5420-7. doi: 10.1523/JNEUROSCI.15-07-05420.1995.

Abstract

The phenotypically plastic neurons of the embryonic mouse striatum were used to explore mechanisms of catecholamine differentiation in culture. De novo transcription and translation of the CA biosynthetic enzyme, tyrosine hydroxylase (TH), was induced in striatal neurons exposed, simultaneously or sequentially, to the growth factor, acidic fibroblast growth factor (aFGF) and a catecholamine. Although dopamine was the most potent aFGF partner (ED50 = 4 microM), a number of substances, including dopamine (D1) receptor agonists, beta-adrenoceptor agonists, and dopamine uptake inhibitors also trigger TH induction when accompanied by aFGF. However, since none of the receptor antagonists nor transport blockers tested could inhibit dopamine's action, the mechanism remains obscure. Structure-activity analysis suggests that effective aFGF partners all contain an amine group separated from a catechol nucleus by two carbons. Thus, TH expression can be novelly induced by the synergistic interaction of aFGF, and to a lesser extent basic FGF, and a variety of CA-containing partner molecules. We speculate that a similar association between growth factor and transmitter may be required in development for the differentiation of a CA phenotype in brain neurons.

摘要

利用胚胎小鼠纹状体中表型可塑性神经元来探究培养物中儿茶酚胺分化的机制。在同时或先后暴露于生长因子酸性成纤维细胞生长因子(aFGF)和儿茶酚胺的纹状体神经元中,诱导了儿茶酚胺生物合成酶酪氨酸羟化酶(TH)的从头转录和翻译。尽管多巴胺是最有效的aFGF伙伴(半数有效浓度ED50 = 4 microM),但包括多巴胺(D1)受体激动剂、β-肾上腺素能受体激动剂和多巴胺摄取抑制剂在内的许多物质,在与aFGF同时存在时也会触发TH诱导。然而,由于所测试的受体拮抗剂和转运阻滞剂均不能抑制多巴胺的作用,其机制仍不清楚。构效分析表明,有效的aFGF伙伴均含有一个与儿茶酚核被两个碳原子隔开的胺基。因此,TH表达可通过aFGF以及在较小程度上碱性FGF与多种含儿茶酚胺伙伴分子的协同相互作用而被新诱导。我们推测,在发育过程中,脑神经元中儿茶酚胺表型的分化可能需要生长因子与递质之间有类似的关联。

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