4.4 Article

Subthalamic deep brain stimulation of an anatomically detailed model of the human hyperdirect pathway

期刊

JOURNAL OF NEUROPHYSIOLOGY
卷 127, 期 5, 页码 1209-1220

出版社

AMER PHYSIOLOGICAL SOC
DOI: 10.1152/jn.00004.2022

关键词

axon; basal ganglia; deep brain stimulation; motor cortex; subthalamic nucleus

资金

  1. National Institutes of Health [R01 NS105690, R01 NS119520]

向作者/读者索取更多资源

This study used biophysical models to investigate the recruitment pathways and conduction latencies of the hyperdirect pathway (HDP) in response to subthalamic deep brain stimulation (DBS). The results suggest that HDP activation is influenced by complex axonal branching in the subthalamic nucleus (STN). These findings provide valuable information for linking HDP activation with evoked potentials (EPs) recorded in clinical experiments.
The motor hyperdirect pathway (HDP) is considered a key target in the treatment of Parkinson's disease with subthalamic deep brain stimulation (DBS). This hypothesis is partially derived from the association of HDP activation with evoked potentials (EPs) generated in the motor cortex and subthalamic nucleus (STN) after a DBS pulse. However, the biophysical details of how and when DBS-induced action potentials (APs) in HDP neurons reach their terminations in the cortex or STN remain unclear. Therefore, we used an anatomically detailed representation of the motor HDP, as well as the internal capsule (IC), in a model of human subthalamic DBS to explore AP activation and transmission in the HDP and IC. Our results show that small diameter HDP axons exhibited AP initiation in their subthalamic terminal arbor, which resulted in relatively long transmission latencies to cortex (similar to 3.5-8 ms). Alternatively, large diameter HDP axons were most likely to be directly activated in the capsular region, which resulted in short transmission times to the cortex (similar to 1-3 ms). However, those large diameter HDP antidromic APs would be indistinguishable from any other IC axons that were also activated by the stimulus. Conversely, DBS-induced APs in both small and large diameter HDP axons reached their synaptic boutons in the STN with similar timings, but both spanned a wide temporal range (similar to 0.5-5 ms). We also found that using anodic or bipolar stimulation helped to bias activation of the HDP over the IC. These computational results provide useful information for linking HDP activation with EP recordings in clinical experiments. NEW & NOTEWORTHY We used biophysical models to study pathway recruitment and conduction latencies of the hyperdirect pathway (HDP) in response to subthalamic deep brain stimulation (DBS). The model system allowed us to assess the influence of increased anatomic& realism on pathway activity and the possibility of identifying HDP activity in evoked potentials (EPs) recorded in either the subthalamic nucleus (STN) or cortex. The model predicts that HDP activation is accentuated by complex axonal branching in the STN.

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