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首页> 外文期刊>Cell transplantation >The release of excitatory amino acids, dopamine, and potassium following transplantation of embryonic mesencephalic dopaminergic grafts to the rat striatum, and their effects on dopaminergic neuronal survival in vitro.
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The release of excitatory amino acids, dopamine, and potassium following transplantation of embryonic mesencephalic dopaminergic grafts to the rat striatum, and their effects on dopaminergic neuronal survival in vitro.

机译:胚胎中脑多巴胺能移植物移植到大鼠纹状体后,兴奋性氨基酸,多巴胺和钾的释放及其对体外多巴胺能神经元存活的影响。

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A major limitation to the effectiveness of grafts of fetal ventral mesencephalic tissue for parkinsonism is that about 90-95% of grafted dopaminergic neurones die. In rats, many of the cells are dead within 1 day and most cell death is complete within 1 week. Our previous results suggest that a major cause of this cell death is the release of toxins from the injured CNS tissue surrounding the graft, and that many of these toxins have dissipated within 1 h of inserting the grafting cannula. In the present experiments we measured the change over time in the concentration of several potential toxins around an acutely implanted grafting cannula. We also measured the additional effect of injecting suspensions of embryonic mesencephalon, latex microspheres, or vehicle on these concentrations. Measurements of glutamate, aspartate, and dopamine by microdialysis showed elevated levels during the first 20-60 min, which then declined to baseline. In the first 20 min glutamate levels were 10.7 times, aspartate levels 5 times, and dopamine levels 24.3 times baseline. Potassium levels increased to a peak of 33 +/- 10.6 mM 4-5 min after cannula insertion, returning to baseline of <5 mM by 30 min. Injection of cell suspension, latex microspheres, or vehicle had no significant effect on these levels. We then assayed the effect of high concentrations of glutamate, aspartate, dopamine, and potassium on dopaminergic neuronal survival in E14 ventral mesencephalic cultures. In monolayer cultures only dopamine at 200 microM showed toxicity. In three-dimensional cultures only the combination of raised potassium, dopamine, glutamate, and aspartate together decreased dopaminergic neuronal survival. We conclude that toxins other than the ones measured are the main cause of dopaminergic cell death after transplantation, or the effects of the toxins measured are enhanced by anoxia and metabolic challenges affecting newly inserted grafts.
机译:胎儿腹侧中脑组织移植物对帕金森病的有效性的主要限制是,约有90-95%的移植的多巴胺能神经元死亡。在大鼠中,许多细胞在1天内死亡,大多数细胞在1周内死亡。我们以前的结果表明,这种细胞死亡的主要原因是毒素从移植物周围受损的CNS组织中释放出来,并且许多这些毒素在插入移植套管后1小时内就消失了。在本实验中,我们测量了急性植入的插管周围几种潜在毒素的浓度随时间的变化。我们还测量了注射胚胎中脑,乳胶微球或赋形剂悬浮液对这些浓度的附加影响。通过微透析测量的谷氨酸,天冬氨酸和多巴胺显示在前20-60分钟内水平升高,然后下降至基线。在最初的20分钟内,谷氨酸水平是基线的10.7倍,天冬氨酸水平是5倍,多巴胺水平是24.3倍。插管插入4-5分钟后,钾水平升高至33 +/- 10.6 mM的峰值,到30分钟时恢复至<5 mM的基线。细胞悬液,乳胶微球或溶媒的注射对这些水平无明显影响。然后,我们分析了高浓度谷氨酸,天冬氨酸,多巴胺和钾对E14腹侧中脑培养物中多巴胺能神经元存活的影响。在单层培养物中,仅200 microM的多巴胺表现出毒性。在三维培养中,仅升高的钾,多巴胺,谷氨酸和天冬氨酸的组合在一起会降低多巴胺能神经元的存活率。我们得出的结论是,所测毒素以外的毒素是移植后多巴胺能细胞死亡的主要原因,或者缺氧和代谢挑战会影响新插入的移植物,从而增强所测毒素的作用。

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