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多巴胺激动剂溴隐亭、培高利特、卡麦角林和SKF-38393对培养的小鼠星形胶质细胞中胶质细胞源性神经营因子(GDNF)、神经生长因子(NGF)和脑源性神经营因子(BDNF)合成的影响。

Effects of dopamine agonists bromocriptine, pergolide, cabergoline, and SKF-38393 on GDNF, NGF, and BDNF synthesis in cultured mouse astrocytes.

作者信息

Ohta Kiyoe, Kuno Sadako, Mizuta Ikuko, Fujinami Aya, Matsui Hidehito, Ohta Mitsuhiro

机构信息

Clinical Research Center, Utano National Hospital, Ukyo-ku, Kyoto 616-8255, Japan.

出版信息

Life Sci. 2003 Jun 20;73(5):617-26. doi: 10.1016/s0024-3205(03)00321-7.

Abstract

We examined the stimulatory effects of the dopamine agonists bromocriptine, pergolide, cabergoline, and SKF-38393 on the synthesis and secretion of neurotrophic factors (nerve growth factor, NGF; brain-derived neurotrophic factor, BDNF; and glial cell line-derived neurotrophic factor, GDNF) in cultured mouse astrocytes, and clarified the role of dopamine D1 and D2 receptors in these effects. Bromocriptine, a D2 agonist, elevated NGF levels in the culture medium 6.8-fold vs. control, and significantly decreased GDNF and BDNF levels, at 24 h. Both pergolide, a D1/D2 agonist, and cabergoline, a D2/weak D1 agonist, rapidly elevated NGF and GDNF levels at 4-6 h, respectively to 21- and 1.5-fold, respectively, and 84- and 9-fold, respectively, of control levels at 24 h. SKF-38393, a D1 agonist, elevated NGF and GDNF levels to 20- and 2.8-fold of controls, respectively, at 24 h. Relative levels of NGF and GDNF mRNA detected by Northern blot analysis or semiquantitative reverse transcriptase-polymerase chain reaction confirmed that increases in levels of the 2 proteins in culture medium were due to overexpression as opposed to leakage from cells. Cabergoline rapidly increased GDNF mRNA expression at 4 h, producing a potent and long-lasting increase in GDNF levels. Bromocriptine significantly suppressed GDNF synthesis. These findings suggest that stimulation of dopamine D1 receptors may be required for GDNF synthesis and secretion, and that concurrent stimulation of dopamine D1 and D2 receptors may augment synthesis and secretion of NGF and GDNF. These dopamine agonists may play a role in neuronal survival by stimulating NGF and GDNF synthesis in the brain, and as drugs are good candidates as NGF and GDNF inducers.

摘要

我们研究了多巴胺激动剂溴隐亭、培高利特、卡麦角林和SKF-38393对培养的小鼠星形胶质细胞中神经营养因子(神经生长因子,NGF;脑源性神经营养因子,BDNF;以及胶质细胞系源性神经营养因子,GDNF)合成和分泌的刺激作用,并阐明了多巴胺D1和D2受体在这些作用中的角色。D2激动剂溴隐亭使24小时时培养基中的NGF水平相对于对照升高了6.8倍,并显著降低了GDNF和BDNF水平。D1/D2激动剂培高利特和D2/弱D1激动剂卡麦角林分别在4 - 6小时迅速升高了NGF和GDNF水平,在24小时时分别达到对照水平的21倍和1.5倍,以及84倍和9倍。D1激动剂SKF-38393在24小时时使NGF和GDNF水平分别升高至对照的20倍和2.8倍。通过Northern印迹分析或半定量逆转录聚合酶链反应检测到的NGF和GDNF mRNA的相对水平证实,培养基中这两种蛋白质水平的升高是由于过表达而非细胞渗漏所致。卡麦角林在4小时时迅速增加了GDNF mRNA表达,使GDNF水平产生了强大而持久的升高。溴隐亭显著抑制了GDNF合成。这些发现表明,GDNF的合成和分泌可能需要多巴胺D1受体的刺激,并且多巴胺D1和D2受体的同时刺激可能增强NGF和GDNF的合成和分泌。这些多巴胺激动剂可能通过刺激脑中NGF和GDNF的合成在神经元存活中发挥作用,并且作为药物是NGF和GDNF诱导剂的良好候选者。

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