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首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Activation of dopamine cell firing by repeated L-DOPA administration to dopamine-depleted rats: its potential role in mediating the therapeutic response to L-DOPA treatment.
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Activation of dopamine cell firing by repeated L-DOPA administration to dopamine-depleted rats: its potential role in mediating the therapeutic response to L-DOPA treatment.

机译:通过向贫多巴胺的大鼠重复施用L-DOPA激活多巴胺细胞放电:其在介导对L-DOPA治疗的治疗反应中的潜在作用。

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摘要

The administration of L-dihydroxyphenylalanine (L-DOPA) to patients with Parkinson's disease is known to produce acute effects that include the reduction of rigidity as well as delayed therapeutic actions involving the resumption of complex motor behavior. In order to examine the potential role of dopamine (DA) cell activity in mediating these responses, the effects of acute and repeated L-DOPA administration on the electrophysiological activity of the residual dopamine (DA) neurons were examined in rats that had received partial 6-hydroxydopamine (6-OHDA)-induced DA lesions. DA cell activity was assessed along three dimensions: (1) the relative proportion of DA neurons exhibiting spontaneous spike firing, (2) their basal firing rate, and (3) their firing pattern. Following 6-OHDA-induced DA depletion, rats were treated for 1 month with saline or L-DOPA. In addition, rats from each group received either an acute injection of L-DOPA or saline on the day of recording. In rats receiving repeated saline treatment, the DA neurons recorded following acute L-DOPA administration were firing at significantly slower basal firing rates and exhibited less burst firing when compared to saline-pretreated rats given acute saline. In contrast, DA cells recorded from rats that had received repeated L-DOPA administration for 4 weeks followed by an acute saline injection did not exhibit any significant differences from DA cells of intact control rats with respect to basal firing rate or firing pattern; however, there was a substantial increase in the proportion of DA neurons exhibiting spontaneous spike firing after correcting for 6-OHDA-induced cell loss. In addition, in rats receiving repeated L-DOPA treatment, the DA cells recorded following acute administration of L-DOPA showed significantly less of a reduction in firing rate when compared to the cells recorded following acute L-DOPA in the saline treatment group. These results show that: (1) acute L-DOPA administration appears to exert its actions by DA autoreceptor stimulation, whereas (2) repeated L-DOPA administration increases the proportion of spontaneously active DA neurons in partially lesioned rats. As a result, repeated L-DOPA administration would be expected to cause an increase in spike-dependent DA release as a consequence of the greater proportion of DA cells showing spontaneous activity. This may be the major factor underlying the delayed therapeutic benefits of L-DOPA therapy in the treatment of Parkinson's disease.
机译:已知对患有帕金森氏病的患者服用L-二羟基苯丙氨酸(L-DOPA)会产生急性效应,包括僵硬性降低以及涉及恢复复杂运动行为的延迟治疗作用。为了检查多巴胺(DA)细胞活性在介导这些反应中的潜在作用,在接受了部分6的大鼠中检查了急性和反复L-DOPA给药对残余多巴胺(DA)神经元电生理活性的影响。 -羟基多巴胺(6-OHDA)诱导的DA损伤。从以下三个方面评估DA细胞的活性:(1)表现出自发尖峰放电的DA神经元的相对比例;(2)它们的基础放电速率;(3)它们的放电模式。在6-OHDA诱导的DA耗竭后,用盐水或L-DOPA治疗大鼠1个月。此外,每组大鼠在记录当天均接受了L-DOPA的急性注射或生理盐水注射。在接受重复生理盐水处理的大鼠中,与给予急性生理盐水的生理盐水预处理大鼠相比,急性L-DOPA给药后记录的DA神经元以较慢的基础放电速率进行放电,并表现出较少的突发放电。相比之下,在连续注射L-DOPA 4周并进行了急性生理盐水注射的大鼠中记录的DA细胞与基础对照组的DA细胞在基础放电率或放电模式方面没有任何显着差异。然而,校正6-OHDA诱导的细胞丢失后,表现出自发尖峰放电的DA神经元的比例显着增加。另外,在接受反复L-DOPA处理的大鼠中,与盐水处理组中的急性L-DOPA后记录的细胞相比,急性给予L-DOPA后记录的DA细胞显示出降低的放电率。这些结果表明:(1)急性L-DOPA给药似乎是通过DA自体受体刺激发挥作用,而(2)重复L-DOPA给药会增加部分病变大鼠中自发活跃DA神经元的比例。结果,由于较大比例的显示自发活性的DA细胞的结果,预期重复L-DOPA施用会引起刺突依赖性DA释放的增加。这可能是L-DOPA治疗帕金森氏病治疗延迟疗效的主要因素。

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