HIGH-FREQUENCY STIMULATION OF THE SUBTHALAMIC NUCLEUS INHIBITS THE FIRING OF JUXTACELLULAR LABELLED 5-HT-CONTAINING NEURONES

H Hartung; S. K. H. Tan; H. M. W. Steinbusch; Y. Temel; T. Sharp

doi:10.1016/j.neuroscience.2011.04.004

HIGH-FREQUENCY STIMULATION OF THE SUBTHALAMIC NUCLEUS INHIBITS THE FIRING OF JUXTACELLULAR LABELLED 5-HT-CONTAINING NEURONES

H Hartung, S. K. H. Tan, H. M. W. Steinbusch, Y. Temel, T. Sharp^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

High-frequency stimulation (HFS) of the subthalamic nucleus (STN) is an established neurosurgical therapy for movement disability in advanced Parkinson's disease (PD), but some patients experience psychiatric side-effects like depression. In a previous electrophysiological study, we observed that HFS of the STN inhibited a population of neurones in the rat dorsal raphe nucleus (DRN), with firing properties characteristic of 5-HT neurones. The present study extended these findings to a second population of neurones, and combined extracellular recording with juxtacellular-labelling to investigate the chemical identity of the neurones affected by HFS. Bilateral HFS (130 Hz, 100-200 mu A, 5 min) of the STN inhibited (26.0 +/- 2.9%) the firing of 37/74 DRN neurones displaying a slow, regular firing pattern. Slower firing neurones were more strongly inhibited than those firing faster. Importantly, 10 inhibited DRN neurones were juxtacellular-labelled with neurobiotin, and all neurones contained 5-HT as shown by post-mortem 5-HT immunocytochemistry. A minority of slow firing DRN neurones (18/74) were activated by STN HFS (37.9 +/- 8.3%) which was not observed previously. Of these neurones, three were juxtacellular-labelled and one was 5-HT immunopositive. Also a small number of DRN neurones (19/74) did not respond to HFS, four of which were juxtacellular-labelled and all contained 5-HT. These data show that individual chemically-identified 5-HT-containing neurones in the DRN were modulated by STN HFS, and that the majority were inhibited but some were activated and some failed to respond. These data extend previous findings of modulation of the 5-HT system by STN HFS but suggest a destabilisation of the 5-HT system rather than simple inhibition as indicated previously. Although the mechanism is not yet known, such changes may contribute to the psychiatric side-effects of STN stimulation in some PD patients.

Original language	English
Pages (from-to)	135-145
Journal	Neuroscience
Volume	186
DOIs	https://doi.org/10.1016/j.neuroscience.2011.04.004
Publication status	Published - 14 Jun 2011

Keywords

deep brain stimulation
Parkinson's disease
depression
5-HT
dorsal raphe nucleus
in vivo electrophysiology

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10.1016/j.neuroscience.2011.04.004

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@article{b00f571df0344569966e8fd22dd677b0,

title = "HIGH-FREQUENCY STIMULATION OF THE SUBTHALAMIC NUCLEUS INHIBITS THE FIRING OF JUXTACELLULAR LABELLED 5-HT-CONTAINING NEURONES",

abstract = "High-frequency stimulation (HFS) of the subthalamic nucleus (STN) is an established neurosurgical therapy for movement disability in advanced Parkinson's disease (PD), but some patients experience psychiatric side-effects like depression. In a previous electrophysiological study, we observed that HFS of the STN inhibited a population of neurones in the rat dorsal raphe nucleus (DRN), with firing properties characteristic of 5-HT neurones. The present study extended these findings to a second population of neurones, and combined extracellular recording with juxtacellular-labelling to investigate the chemical identity of the neurones affected by HFS. Bilateral HFS (130 Hz, 100-200 mu A, 5 min) of the STN inhibited (26.0 +/- 2.9%) the firing of 37/74 DRN neurones displaying a slow, regular firing pattern. Slower firing neurones were more strongly inhibited than those firing faster. Importantly, 10 inhibited DRN neurones were juxtacellular-labelled with neurobiotin, and all neurones contained 5-HT as shown by post-mortem 5-HT immunocytochemistry. A minority of slow firing DRN neurones (18/74) were activated by STN HFS (37.9 +/- 8.3%) which was not observed previously. Of these neurones, three were juxtacellular-labelled and one was 5-HT immunopositive. Also a small number of DRN neurones (19/74) did not respond to HFS, four of which were juxtacellular-labelled and all contained 5-HT. These data show that individual chemically-identified 5-HT-containing neurones in the DRN were modulated by STN HFS, and that the majority were inhibited but some were activated and some failed to respond. These data extend previous findings of modulation of the 5-HT system by STN HFS but suggest a destabilisation of the 5-HT system rather than simple inhibition as indicated previously. Although the mechanism is not yet known, such changes may contribute to the psychiatric side-effects of STN stimulation in some PD patients. ",

keywords = "deep brain stimulation, Parkinson's disease, depression, 5-HT, dorsal raphe nucleus, in vivo electrophysiology",

author = "H Hartung and Tan, {S. K. H.} and Steinbusch, {H. M. W.} and Y. Temel and T. Sharp",

year = "2011",

month = jun,

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doi = "10.1016/j.neuroscience.2011.04.004",

language = "English",

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journal = "Neuroscience",

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T1 - HIGH-FREQUENCY STIMULATION OF THE SUBTHALAMIC NUCLEUS INHIBITS THE FIRING OF JUXTACELLULAR LABELLED 5-HT-CONTAINING NEURONES

AU - Hartung, H

AU - Tan, S. K. H.

AU - Steinbusch, H. M. W.

AU - Temel, Y.

AU - Sharp, T.

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N2 - High-frequency stimulation (HFS) of the subthalamic nucleus (STN) is an established neurosurgical therapy for movement disability in advanced Parkinson's disease (PD), but some patients experience psychiatric side-effects like depression. In a previous electrophysiological study, we observed that HFS of the STN inhibited a population of neurones in the rat dorsal raphe nucleus (DRN), with firing properties characteristic of 5-HT neurones. The present study extended these findings to a second population of neurones, and combined extracellular recording with juxtacellular-labelling to investigate the chemical identity of the neurones affected by HFS. Bilateral HFS (130 Hz, 100-200 mu A, 5 min) of the STN inhibited (26.0 +/- 2.9%) the firing of 37/74 DRN neurones displaying a slow, regular firing pattern. Slower firing neurones were more strongly inhibited than those firing faster. Importantly, 10 inhibited DRN neurones were juxtacellular-labelled with neurobiotin, and all neurones contained 5-HT as shown by post-mortem 5-HT immunocytochemistry. A minority of slow firing DRN neurones (18/74) were activated by STN HFS (37.9 +/- 8.3%) which was not observed previously. Of these neurones, three were juxtacellular-labelled and one was 5-HT immunopositive. Also a small number of DRN neurones (19/74) did not respond to HFS, four of which were juxtacellular-labelled and all contained 5-HT. These data show that individual chemically-identified 5-HT-containing neurones in the DRN were modulated by STN HFS, and that the majority were inhibited but some were activated and some failed to respond. These data extend previous findings of modulation of the 5-HT system by STN HFS but suggest a destabilisation of the 5-HT system rather than simple inhibition as indicated previously. Although the mechanism is not yet known, such changes may contribute to the psychiatric side-effects of STN stimulation in some PD patients.

AB - High-frequency stimulation (HFS) of the subthalamic nucleus (STN) is an established neurosurgical therapy for movement disability in advanced Parkinson's disease (PD), but some patients experience psychiatric side-effects like depression. In a previous electrophysiological study, we observed that HFS of the STN inhibited a population of neurones in the rat dorsal raphe nucleus (DRN), with firing properties characteristic of 5-HT neurones. The present study extended these findings to a second population of neurones, and combined extracellular recording with juxtacellular-labelling to investigate the chemical identity of the neurones affected by HFS. Bilateral HFS (130 Hz, 100-200 mu A, 5 min) of the STN inhibited (26.0 +/- 2.9%) the firing of 37/74 DRN neurones displaying a slow, regular firing pattern. Slower firing neurones were more strongly inhibited than those firing faster. Importantly, 10 inhibited DRN neurones were juxtacellular-labelled with neurobiotin, and all neurones contained 5-HT as shown by post-mortem 5-HT immunocytochemistry. A minority of slow firing DRN neurones (18/74) were activated by STN HFS (37.9 +/- 8.3%) which was not observed previously. Of these neurones, three were juxtacellular-labelled and one was 5-HT immunopositive. Also a small number of DRN neurones (19/74) did not respond to HFS, four of which were juxtacellular-labelled and all contained 5-HT. These data show that individual chemically-identified 5-HT-containing neurones in the DRN were modulated by STN HFS, and that the majority were inhibited but some were activated and some failed to respond. These data extend previous findings of modulation of the 5-HT system by STN HFS but suggest a destabilisation of the 5-HT system rather than simple inhibition as indicated previously. Although the mechanism is not yet known, such changes may contribute to the psychiatric side-effects of STN stimulation in some PD patients.

KW - deep brain stimulation

KW - Parkinson's disease

KW - depression

KW - 5-HT

KW - dorsal raphe nucleus

KW - in vivo electrophysiology

U2 - 10.1016/j.neuroscience.2011.04.004

DO - 10.1016/j.neuroscience.2011.04.004

M3 - Article

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SN - 0306-4522

VL - 186

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JO - Neuroscience

JF - Neuroscience

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