Impulse-dependent extracellular resting dopamine concentration in rat striatum in vivo

Pan Li Zuo; Wei Yao; Liang Sun; Shu Ting Kuo; Qing Li; Shi Rong Wang; Hai Qiang Dou; Hua Dong Xu; Claire Xi Zhang; Xin Jiang Kang; Zhuan Zhou; Bo Zhang

doi:10.1016/j.neuint.2012.11.006

Impulse-dependent extracellular resting dopamine concentration in rat striatum in vivo

Pan Li Zuo, Wei Yao, Liang Sun, Shu Ting Kuo, Qing Li, Shi Rong Wang, Hai Qiang Dou, Hua Dong Xu, Claire Xi Zhang, Xin Jiang Kang, Zhuan Zhou^*, Bo Zhang

^*Corresponding author for this work

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

4 Citations (Scopus)

Abstract

The ambient resting dopamine (DA) concentration in brain regulates cognition and motivation. Despite its importance, resting DA level in vivo remains elusive. Here, by high-frequency stimulation of the medial forebrain bundle and immediately following the stimulus-induced DA overflow, we recorded a DA "undershoot" which is a temporal reduction of DA concentration to a level below the baseline. Based on the DA undershoot, we predicted a resting DA concentration of ∼73 nM in rat striatum in vivo. Simulation studies suggested that removing basal DA by DAT during the post-stimulation inhibition of tonic DA release caused the DA undershoot, and the resting concentration of DA modulated the kinetics of the evoked DA transient. The DA undershoot was eliminated by either blocking D2 receptors with haloperidol or blocking the DA transporter (DAT) with cocaine. Therefore, the impulse-dependent resting DA concentration is in the tens of nanomolar range and is modulated by the presynaptic D2 receptors and the DAT in vivo.

Original language	English
Pages (from-to)	50-57
Number of pages	8
Journal	Neurochemistry International
Volume	62
Issue number	1
DOIs	https://doi.org/10.1016/j.neuint.2012.11.006
Publication status	Published - Jan 2013
Externally published	Yes

Keywords

Amperometry
D2 receptors
In vivo
Resting dopamine
Striatum
Undershoot

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10.1016/j.neuint.2012.11.006

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title = "Impulse-dependent extracellular resting dopamine concentration in rat striatum in vivo",

abstract = "The ambient resting dopamine (DA) concentration in brain regulates cognition and motivation. Despite its importance, resting DA level in vivo remains elusive. Here, by high-frequency stimulation of the medial forebrain bundle and immediately following the stimulus-induced DA overflow, we recorded a DA {"}undershoot{"} which is a temporal reduction of DA concentration to a level below the baseline. Based on the DA undershoot, we predicted a resting DA concentration of ∼73 nM in rat striatum in vivo. Simulation studies suggested that removing basal DA by DAT during the post-stimulation inhibition of tonic DA release caused the DA undershoot, and the resting concentration of DA modulated the kinetics of the evoked DA transient. The DA undershoot was eliminated by either blocking D2 receptors with haloperidol or blocking the DA transporter (DAT) with cocaine. Therefore, the impulse-dependent resting DA concentration is in the tens of nanomolar range and is modulated by the presynaptic D2 receptors and the DAT in vivo.",

keywords = "Amperometry, D2 receptors, In vivo, Resting dopamine, Striatum, Undershoot",

author = "Zuo, {Pan Li} and Wei Yao and Liang Sun and Kuo, {Shu Ting} and Qing Li and Wang, {Shi Rong} and Dou, {Hai Qiang} and Xu, {Hua Dong} and Zhang, {Claire Xi} and Kang, {Xin Jiang} and Zhuan Zhou and Bo Zhang",

note = "Funding Information: We thank Dr. Iain Bruce for comments on manuscript. This work was supported by Grants from the National Basic Research Program of China (2012CB518006), the National Natural Science Foundation of China (31221002, 31228010, 31171026, 31100597, 30970660, 30911120491 and 30830043), and a “985” Grant from the Department of Education of China. ",

year = "2013",

month = jan,

doi = "10.1016/j.neuint.2012.11.006",

language = "English",

volume = "62",

pages = "50--57",

journal = "Neurochemistry International",

issn = "0197-0186",

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T1 - Impulse-dependent extracellular resting dopamine concentration in rat striatum in vivo

AU - Zuo, Pan Li

AU - Yao, Wei

AU - Sun, Liang

AU - Kuo, Shu Ting

AU - Li, Qing

AU - Wang, Shi Rong

AU - Dou, Hai Qiang

AU - Xu, Hua Dong

AU - Zhang, Claire Xi

AU - Kang, Xin Jiang

AU - Zhou, Zhuan

AU - Zhang, Bo

N1 - Funding Information: We thank Dr. Iain Bruce for comments on manuscript. This work was supported by Grants from the National Basic Research Program of China (2012CB518006), the National Natural Science Foundation of China (31221002, 31228010, 31171026, 31100597, 30970660, 30911120491 and 30830043), and a “985” Grant from the Department of Education of China.

PY - 2013/1

Y1 - 2013/1

N2 - The ambient resting dopamine (DA) concentration in brain regulates cognition and motivation. Despite its importance, resting DA level in vivo remains elusive. Here, by high-frequency stimulation of the medial forebrain bundle and immediately following the stimulus-induced DA overflow, we recorded a DA "undershoot" which is a temporal reduction of DA concentration to a level below the baseline. Based on the DA undershoot, we predicted a resting DA concentration of ∼73 nM in rat striatum in vivo. Simulation studies suggested that removing basal DA by DAT during the post-stimulation inhibition of tonic DA release caused the DA undershoot, and the resting concentration of DA modulated the kinetics of the evoked DA transient. The DA undershoot was eliminated by either blocking D2 receptors with haloperidol or blocking the DA transporter (DAT) with cocaine. Therefore, the impulse-dependent resting DA concentration is in the tens of nanomolar range and is modulated by the presynaptic D2 receptors and the DAT in vivo.

AB - The ambient resting dopamine (DA) concentration in brain regulates cognition and motivation. Despite its importance, resting DA level in vivo remains elusive. Here, by high-frequency stimulation of the medial forebrain bundle and immediately following the stimulus-induced DA overflow, we recorded a DA "undershoot" which is a temporal reduction of DA concentration to a level below the baseline. Based on the DA undershoot, we predicted a resting DA concentration of ∼73 nM in rat striatum in vivo. Simulation studies suggested that removing basal DA by DAT during the post-stimulation inhibition of tonic DA release caused the DA undershoot, and the resting concentration of DA modulated the kinetics of the evoked DA transient. The DA undershoot was eliminated by either blocking D2 receptors with haloperidol or blocking the DA transporter (DAT) with cocaine. Therefore, the impulse-dependent resting DA concentration is in the tens of nanomolar range and is modulated by the presynaptic D2 receptors and the DAT in vivo.

KW - Amperometry

KW - D2 receptors

KW - In vivo

KW - Resting dopamine

KW - Striatum

KW - Undershoot

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Impulse-dependent extracellular resting dopamine concentration in rat striatum in vivo

Abstract

Keywords

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