The role of beta-arrestin2 in shaping fMRI BOLD responses to dopaminergic stimulation

Sahlholm, Kristoffer; Ielacqua, Giovanna D.; Xu, Jinbin; Jones, Lynne A.; Schlegel, Felix; Mach, Robert H.; Rudin, Markus; Schroeter, Aileen

doi:https://doi.org/10.3929/ethz-b-000237488

The role of beta-arrestin2 in shaping fMRI BOLD responses to dopaminergic stimulation

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Author / Producer

Sahlholm, Kristoffer

Ielacqua, Giovanna D.

Xu, Jinbin

Date

2017-07

Publication Type

Journal Article

ETH Bibliography

yes

OPEN ACCESS

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Creative Commons Attribution 4.0 International north_east

Abstract

Rationale The dopamine D2 receptor (D2R) couples to inhibitory Gi/o proteins and is targeted by antipsychotic and antiparkinsonian drugs. Beta-arrestin2 binds to the intracellular regions of the agonist-occupied D2R to terminate G protein activation and promote internalization, but also to initiate downstream signaling cascades which have been implicated in psychosis. Functional magnetic resonance imaging (fMRI) has proven valuable for measuring dopamine receptor-mediated changes in neuronal activity, and might enable beta-arrestin2 function to be studied in vivo. Objectives The present study examined fMRI blood oxygenation level dependent (BOLD) signal changes elicited by a dopamine agonist in wild-type (WT) and beta-arrestin2 knockout (KO) mice, to investigate whether genetic deletion of beta-arrestin2 prolongs or otherwise modifies D2R-dependent responses. Methods fMRI BOLD data were acquired on a 9.4 T system. During scans, animals received 0.2 mg/kg apomorphine, i.v. In a subset of experiments, animals were pretreated with 2 mg/kg of the D2R antagonist, eticlopride. Results Following apomorphine administration, BOLD signal decreases were observed in caudate/putamen of WT and KO animals. The time course of response decay in caudate/putamen was significantly slower in KO vs. WT animals. In cingulate cortex, an initial BOLD signal decrease was followed by a positive response component in WT but not in KO animals. Eticlopride pretreatment significantly reduced apomorphine-induced BOLD signal changes. Conclusions The prolonged striatal response decay rates in KO animals might reflect impaired D2R desensitization, consistent with the known function of beta-arrestin2. Furthermore, the apomorphine-induced positive response component in cingulate cortex may depend on beta-arrestin2 signaling downstream of D2R.

Permanent link

https://doi.org/10.3929/ethz-b-000237488

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published

External links

https://doi.org/10.1007/s00213-017-4609-6 north_east

Journal / series

Psychopharmacology north_east

Volume

234 (13)

Pages / Article No.

2019 - 2030

Publisher

Springer

Subject

Arrestin3; Dopamine; Dopamine receptor; Dopamine agents; Eticlopride

Organisational unit

03750 - Rudin, Markus (emeritus) check_circle

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The role of beta-arrestin2 in shaping fMRI BOLD responses to dopaminergic stimulation

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