单次电刺激诱发反应揭示帕金森病大鼠模型纹状体兴奋性受损。
Evoked responses to single pulse electrical stimulation reveal impaired striatal excitability in a rat model of Parkinson's disease.
机构信息
SynapCell SAS, Saint-Ismier, France; Univ. Grenoble Alpes, Inserm, U1216, Grenoble Institut Neurosciences, 38000 Grenoble, France.
SynapCell SAS, Saint-Ismier, France.
出版信息
Neurobiol Dis. 2023 Sep;185:106266. doi: 10.1016/j.nbd.2023.106266. Epub 2023 Aug 19.
BACKGROUND
Sensorimotor beta oscillations are increased in Parkinson's disease (PD) due to the alteration of dopaminergic transmission. This electrophysiological read-out is reported both in patients and in animal models such as the 6-OHDA rat model obtained with unilateral nigral injection of 6-hydroxydopamine (6-OHDA). Current treatments, based on dopaminergic replacement, transiently normalize this pathological beta activity and improve patients' quality of life.
OBJECTIVES
We wanted to assess in vivo whether the abnormal beta oscillations can be correlated with impaired striatal or cortical excitability of the sensorimotor system and modulated by the pharmacological manipulation of the dopaminergic system.
METHODS
In the unilateral 6-OHDA rat model and control animals, we used intra-striatal and intra-cortical single-pulse electrical stimulation (SPES) and concurrent local field potentials (LFP) recordings. In the two groups, we quantified basal cortico-striatal excitability from time-resolved spectral analyses of LFP evoked responses induced remotely by intracerebral stimulations. The temporal dependance of cortico-striatal excitability to dopaminergic transmission was further tested using electrophysiological recordings combined with levodopa injection.
RESULTS
LFP evoked responses after striatal stimulation showed a transient reduction of power in a large time-frequency domain in the 6-OHDA group compared to the sham group. This result was specific to the striatum, as no significant difference was observed in cortical LFP evoked responses between the two groups. This impaired striatal excitability in the 6-OHDA group was observed in the striatum at least during the first 3 months after the initial lesion. In addition, the striatum responses to SPES during a levodopa challenge showed a transient potentiation of the decrease of responsiveness in frequencies below 40 Hz.
CONCLUSION
The spectral properties of striatal responses to SPES show high sensitivity to dopaminergic transmission in the unilateral 6-OHDA rat model. We thus propose that this approach could be used in preclinical models as a time-resolved biomarker of impaired dopaminergic transmission capable of monitoring progressive neurodegeneration and/or challenges to drug intake.
背景
由于多巴胺能传递的改变,帕金森病(PD)患者的感觉运动β振荡增加。这种电生理读数在患者和动物模型中均有报道,例如通过单侧黑质注射 6-羟多巴胺(6-OHDA)获得的 6-OHDA 大鼠模型。目前基于多巴胺替代的治疗方法暂时使这种病理性β活动正常化,并改善了患者的生活质量。
目的
我们希望在体内评估异常β振荡是否可以与感觉运动系统纹状体或皮质兴奋性受损相关,并通过多巴胺能系统的药理学干预进行调节。
方法
在单侧 6-OHDA 大鼠模型和对照动物中,我们使用纹状体内和皮质内单脉冲电刺激(SPES)和同时的局部场电位(LFP)记录。在两组中,我们通过对由脑内刺激远程诱导的 LFP 诱发反应的时间分辨谱分析,量化基础的纹状皮质兴奋性。使用电生理记录结合左旋多巴注射进一步测试了对多巴胺能传递的皮质纹状体兴奋性的时间依赖性。
结果
与假手术组相比,6-OHDA 组的 LFP 诱发反应在较大的时频域中表现出短暂的功率降低。该结果是纹状体特异性的,因为两组之间皮质 LFP 诱发反应没有显著差异。在初始损伤后至少 3 个月,6-OHDA 组的纹状体兴奋性受损。此外,在左旋多巴挑战期间,SPES 对纹状体的反应表现出对低于 40 Hz 的频率的反应性降低的短暂增强。
结论
SPES 对纹状体反应的频谱特性对单侧 6-OHDA 大鼠模型中的多巴胺能传递具有高灵敏度。因此,我们提出这种方法可以作为一种时间分辨的多巴胺能传递受损的生物标志物,用于临床前模型,能够监测进行性神经退行性变和/或药物摄入的挑战。
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