Literature DB >> 17234435

Modelling the role of excitatory and inhibitory neuronal activity in the generation of the BOLD signal.

Roberto C Sotero1, Nelson J Trujillo-Barreto.   

Abstract

A biophysical model of the coupling between neuronal activity and the BOLD signal that allows for explicitly evaluating the role of both excitatory and inhibitory activity is formulated in this paper. The model is based on several physiological assumptions. Firstly, in addition to glycolysis, the "glycogen shunt" is assumed for excitatory synapses as a mechanism for energy production in the astrocytes. As a result, oxygen-to-glucose index (OGI) is not constant but varies with excitatory neuronal activity. In contrast, a constant OGI=6 (glycolysis) is assumed for inhibitory synapses. Finally we assume that cerebral blood flow is not directly controlled by energy usage, but it is only related to excitatory activity. Simulations' results show that increases in excitatory activity amplify the oscillations associated with the transient BOLD response, by increasing the initial dip, the maximum, and the post-stimulus undershoot of the signal. In contrast, increasing the inhibitory activity evoked an overall decrease of the BOLD signal along the whole time interval of the response. Simultaneous increase of both types of activity is then expected to reinforce the initial dip and the post-stimulus undershoot, while respective effects on the maximum tend to counteract each other. Two mechanisms for negative BOLD response (NBS) generation were predicted by the model: (i) when inhibition was present alone or together with low activation levels and (ii) when deactivation occurred independently of the accompanying inhibition level. Interestingly, NBS was associated with negative oxygen consumption changes only for the case of mechanism (ii).

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Year:  2007        PMID: 17234435     DOI: 10.1016/j.neuroimage.2006.10.027

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


  33 in total

1.  Energy-based stochastic control of neural mass models suggests time-varying effective connectivity in the resting state.

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4.  Frequency-selective control of cortical and subcortical networks by central thalamus.

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5.  Identification and comparison of stochastic metabolic/hemodynamic models (sMHM) for the generation of the BOLD signal.

Authors:  Roberto C Sotero; Nelson J Trujillo-Barreto; Juan C Jiménez; Felix Carbonell; Rafael Rodríguez-Rojas
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6.  Neural substrates underlying the passive observation and active control of translational egomotion.

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7.  Method for spatial overlap estimation of electroencephalography and functional magnetic resonance imaging responses.

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8.  High-resolution BOLD fMRI measurements of local orientation-dependent contextual modulation show a mismatch between predicted V1 output and local BOLD response.

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9.  Electrophysiological effects of non-invasive Radio Electric Asymmetric Conveyor (REAC) on thalamocortical neural activities and perturbed experimental conditions.

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10.  Interneurons contribute to the hemodynamic/metabolic response to epileptiform discharges.

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