4.7 Article

GABA-ergic Dynamics in Human Frontotemporal Networks Confirmed by Pharmaco-Magnetoencephalography

Journal

JOURNAL OF NEUROSCIENCE
Volume 40, Issue 8, Pages 1640-1649

Publisher

SOC NEUROSCIENCE
DOI: 10.1523/JNEUROSCI.1689-19.2019

Keywords

conductance-based model; frontotemporal; GABA; generative modeling; pharmaco-MEG; tonic inhibition

Categories

Funding

  1. Wellcome Trust [103838]
  2. National Institute for Health Research Cambridge Biomedical Research Centre
  3. Medical Research Council [MC_U105597119, MC_U_00005/12, SUAG/004/91365]
  4. Wellcome Trust Strategic Award [104943/Z/14/Z]
  5. Cambridge Centre for Parkinson-plus
  6. Holt Fellowship
  7. MRC [MC_UU_00005/12, MC_U105597119] Funding Source: UKRI

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To bridge the gap between preclinical cellular models of disease and in vivo imaging of human cognitive network dynamics, there is a pressing need for informative biophysical models. Here we assess dynamic causal models (DCM) of cortical network responses, as generative models of magnetoencephalographic observations during an auditory oddball roving paradigm in healthy adults. This paradigm induces robust perturbations that permeate frontotemporal networks, including an evoked 'mismatch negativity' response and transiently induced oscillations. Here, we probe GABAergic influences in the networks using double-blind placebo-controlled randomized-crossover administration of the GABA reuptake inhibitor, tiagabine (oral, 10 mg) in healthy older adults. We demonstrate the facility of conductance-based neural mass mean-field models, incorporating local synaptic connectivity, to investigate laminar-specific and GABAergic mechanisms of the auditory response. The neuronal model accurately recapitulated the observed magnetoencephalographic data. Using parametric empirical Bayes for optimal model inversion across both drug sessions, we identify the effect of tiagabine on GABAergic modulation of deep pyramidal and interneuronal cell populations. We found a transition of the main GABAergic drug effects from auditory cortex in standard trials to prefrontal cortex in deviant trials. The successful integration of pharmaco-magnetoencephalography with dynamic causal models of frontotemporal networks provides a potential platform on which to evaluate the effects of disease and pharmacological interventions.

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