Literature DB >> 23466936

A receptor-based model for dopamine-induced fMRI signal.

Joseph B Mandeville1, Christin Y M Sander2, Bruce G Jenkins3, Jacob M Hooker3, Ciprian Catana3, Wim Vanduffel3, Nathaniel M Alpert4, Bruce R Rosen3, Marc D Normandin4.   

Abstract

This report describes a multi-receptor physiological model of the fMRI temporal response and signal magnitude evoked by drugs that elevate synaptic dopamine in basal ganglia. The model is formulated as a summation of dopamine's effects at D1-like and D2-like receptor families, which produce functional excitation and inhibition, respectively, as measured by molecular indicators like adenylate cyclase or neuroimaging techniques like fMRI. Functional effects within the model are described in terms of relative changes in receptor occupancies scaled by receptor densities and neuro-vascular coupling constants. Using literature parameters, the model reconciles many discrepant observations and interpretations of pre-clinical data. Additionally, we present data showing that amphetamine stimulation produces fMRI inhibition at low doses and a biphasic response at higher doses in the basal ganglia of non-human primates (NHP), in agreement with model predictions based upon the respective levels of evoked dopamine. Because information about dopamine release is required to inform the fMRI model, we simultaneously acquired PET (11)C-raclopride data in several studies to evaluate the relationship between raclopride displacement and assumptions about dopamine release. At high levels of dopamine release, results suggest that refinements of the model will be required to consistently describe the PET and fMRI data. Overall, the remarkable success of the model in describing a wide range of preclinical fMRI data indicate that this approach will be useful for guiding the design and analysis of basic science and clinical investigations and for interpreting the functional consequences of dopaminergic stimulation in normal subjects and in populations with dopaminergic neuroadaptations.
Copyright © 2013 Elsevier Inc. All rights reserved.

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Year:  2013        PMID: 23466936      PMCID: PMC3683121          DOI: 10.1016/j.neuroimage.2013.02.036

Source DB:  PubMed          Journal:  Neuroimage        ISSN: 1053-8119            Impact factor:   6.556


  78 in total

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2.  Mapping dopamine D2/D3 receptor function using pharmacological magnetic resonance imaging.

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3.  Neural correlates of high and craving during cocaine self-administration using BOLD fMRI.

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4.  Dopaminergic activities in the human striatum: rostrocaudal gradients of uptake sites and of D1 and D2 but not of D3 receptor binding or dopamine.

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5.  Demonstration of dose-dependent global and regional cocaine-induced reductions in brain blood flow using a novel approach to quantitative single photon emission computerized tomography.

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Review 7.  Imaging the dopamine system with in vivo [11C]raclopride displacement studies: understanding the true mechanism.

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  31 in total

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Review 2.  From simultaneous to synergistic MR-PET brain imaging: A review of hybrid MR-PET imaging methodologies.

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6.  Abstinence to chronic methamphetamine switches connectivity between striatal, hippocampal and sensorimotor regions and increases cerebral blood volume response.

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Journal:  Neuroimage       Date:  2018-03-05       Impact factor: 6.556

7.  Frequency- and State-Dependent Network Effects of Electrical Stimulation Targeting the Ventral Tegmental Area in Macaques.

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Review 8.  Data collection and analysis strategies for phMRI.

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10.  Dynamic functional imaging of brain glucose utilization using fPET-FDG.

Authors:  Marjorie Villien; Hsiao-Ying Wey; Joseph B Mandeville; Ciprian Catana; Jonathan R Polimeni; Christin Y Sander; Nicole R Zürcher; Daniel B Chonde; Joanna S Fowler; Bruce R Rosen; Jacob M Hooker
Journal:  Neuroimage       Date:  2014-06-14       Impact factor: 6.556

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