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July 16, 2019; 93 (3) Article

The epileptic network of Lennox-Gastaut syndrome

Cortically driven and reproducible across age

View ORCID ProfileAaron E.L. Warren, A. Simon Harvey, Simon J. Vogrin, Catherine Bailey, Andrew Davidson, Graeme D. Jackson, David F. Abbott, John S. Archer
First published June 21, 2019, DOI: https://doi.org/10.1212/WNL.0000000000007775
Aaron E.L. Warren
From the Department of Medicine (Austin Health) (A.E.L.W., G.D.J., D.F.A., J.S.A.), Florey Institute of Neuroscience and Mental Health (A.E.L.W., A.S.H., G.D.J., D.F.A., J.S.A.), and Department of Paediatrics (A.S.H., A.D.), University of Melbourne; Murdoch Children's Research Institute (A.E.L.W., A.S.H., S.J.V., A.D., J.S.A.); Department of Neurology (G.D.J., J.S.A.), Austin Health; and Departments of Neurology (A.S.H., C.B.) and Anaesthesia and Pain Management (A.D.), Royal Children's Hospital, Victoria, Australia.
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  • ORCID record for Aaron E.L. Warren
A. Simon Harvey
From the Department of Medicine (Austin Health) (A.E.L.W., G.D.J., D.F.A., J.S.A.), Florey Institute of Neuroscience and Mental Health (A.E.L.W., A.S.H., G.D.J., D.F.A., J.S.A.), and Department of Paediatrics (A.S.H., A.D.), University of Melbourne; Murdoch Children's Research Institute (A.E.L.W., A.S.H., S.J.V., A.D., J.S.A.); Department of Neurology (G.D.J., J.S.A.), Austin Health; and Departments of Neurology (A.S.H., C.B.) and Anaesthesia and Pain Management (A.D.), Royal Children's Hospital, Victoria, Australia.
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Simon J. Vogrin
From the Department of Medicine (Austin Health) (A.E.L.W., G.D.J., D.F.A., J.S.A.), Florey Institute of Neuroscience and Mental Health (A.E.L.W., A.S.H., G.D.J., D.F.A., J.S.A.), and Department of Paediatrics (A.S.H., A.D.), University of Melbourne; Murdoch Children's Research Institute (A.E.L.W., A.S.H., S.J.V., A.D., J.S.A.); Department of Neurology (G.D.J., J.S.A.), Austin Health; and Departments of Neurology (A.S.H., C.B.) and Anaesthesia and Pain Management (A.D.), Royal Children's Hospital, Victoria, Australia.
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Catherine Bailey
From the Department of Medicine (Austin Health) (A.E.L.W., G.D.J., D.F.A., J.S.A.), Florey Institute of Neuroscience and Mental Health (A.E.L.W., A.S.H., G.D.J., D.F.A., J.S.A.), and Department of Paediatrics (A.S.H., A.D.), University of Melbourne; Murdoch Children's Research Institute (A.E.L.W., A.S.H., S.J.V., A.D., J.S.A.); Department of Neurology (G.D.J., J.S.A.), Austin Health; and Departments of Neurology (A.S.H., C.B.) and Anaesthesia and Pain Management (A.D.), Royal Children's Hospital, Victoria, Australia.
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Andrew Davidson
From the Department of Medicine (Austin Health) (A.E.L.W., G.D.J., D.F.A., J.S.A.), Florey Institute of Neuroscience and Mental Health (A.E.L.W., A.S.H., G.D.J., D.F.A., J.S.A.), and Department of Paediatrics (A.S.H., A.D.), University of Melbourne; Murdoch Children's Research Institute (A.E.L.W., A.S.H., S.J.V., A.D., J.S.A.); Department of Neurology (G.D.J., J.S.A.), Austin Health; and Departments of Neurology (A.S.H., C.B.) and Anaesthesia and Pain Management (A.D.), Royal Children's Hospital, Victoria, Australia.
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Graeme D. Jackson
From the Department of Medicine (Austin Health) (A.E.L.W., G.D.J., D.F.A., J.S.A.), Florey Institute of Neuroscience and Mental Health (A.E.L.W., A.S.H., G.D.J., D.F.A., J.S.A.), and Department of Paediatrics (A.S.H., A.D.), University of Melbourne; Murdoch Children's Research Institute (A.E.L.W., A.S.H., S.J.V., A.D., J.S.A.); Department of Neurology (G.D.J., J.S.A.), Austin Health; and Departments of Neurology (A.S.H., C.B.) and Anaesthesia and Pain Management (A.D.), Royal Children's Hospital, Victoria, Australia.
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David F. Abbott
From the Department of Medicine (Austin Health) (A.E.L.W., G.D.J., D.F.A., J.S.A.), Florey Institute of Neuroscience and Mental Health (A.E.L.W., A.S.H., G.D.J., D.F.A., J.S.A.), and Department of Paediatrics (A.S.H., A.D.), University of Melbourne; Murdoch Children's Research Institute (A.E.L.W., A.S.H., S.J.V., A.D., J.S.A.); Department of Neurology (G.D.J., J.S.A.), Austin Health; and Departments of Neurology (A.S.H., C.B.) and Anaesthesia and Pain Management (A.D.), Royal Children's Hospital, Victoria, Australia.
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John S. Archer
From the Department of Medicine (Austin Health) (A.E.L.W., G.D.J., D.F.A., J.S.A.), Florey Institute of Neuroscience and Mental Health (A.E.L.W., A.S.H., G.D.J., D.F.A., J.S.A.), and Department of Paediatrics (A.S.H., A.D.), University of Melbourne; Murdoch Children's Research Institute (A.E.L.W., A.S.H., S.J.V., A.D., J.S.A.); Department of Neurology (G.D.J., J.S.A.), Austin Health; and Departments of Neurology (A.S.H., C.B.) and Anaesthesia and Pain Management (A.D.), Royal Children's Hospital, Victoria, Australia.
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Citation
The epileptic network of Lennox-Gastaut syndrome
Cortically driven and reproducible across age
Aaron E.L. Warren, A. Simon Harvey, Simon J. Vogrin, Catherine Bailey, Andrew Davidson, Graeme D. Jackson, David F. Abbott, John S. Archer
Neurology Jul 2019, 93 (3) e215-e226; DOI: 10.1212/WNL.0000000000007775

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Abstract

Objective To identify brain regions underlying interictal generalized paroxysmal fast activity (GPFA), and their causal interactions, in children and adults with Lennox-Gastaut syndrome (LGS).

Methods Concurrent scalp EEG-fMRI was performed in 2 separately analyzed patient groups with LGS: 10 children (mean age 8.9 years) scanned under isoflurane-remifentanil anesthesia and 15 older patients (mean age 31.7 years) scanned without anesthesia. Whole-brain event-related analysis determined GPFA-related activation in each group. Results were used as priors in a dynamic causal modeling (DCM) analysis comparing evidence for different neuronal hypotheses describing initiation and propagation of GPFA between cortex, thalamus, and brainstem.

Results A total of 1,045 GPFA events were analyzed (cumulative duration 1,433 seconds). In both pediatric and older groups, activation occurred in distributed association cortical areas, as well as the thalamus and brainstem (p < 0.05, corrected for family-wise error). Activation was similar across individual patients with structural, genetic, and unknown etiologies of epilepsy, particularly in frontoparietal cortex. In both groups, DCM revealed that GPFA was most likely driven by prefrontal cortex, with propagation occurring first to the brainstem and then from brainstem to thalamus.

Conclusions We show reproducible evidence of a cortically driven process within the epileptic network of LGS. This network is present early (in children) and late (in older patients) in the course of the syndrome and across diverse etiologies of epilepsy, suggesting that LGS reflects shared “secondary network” involvement. A cortical-to-subcortical hierarchy is postulated whereby GPFA rapidly propagates from prefrontal cortex to the brainstem via extrapyramidal corticoreticular pathways, whereas the thalamus is engaged secondarily.

Glossary

BOLD=
blood oxygen level–dependent;
DCM=
dynamic causal modeling;
FWE=
family-wise error;
GPFA=
generalized paroxysmal fast activity;
LGS=
Lennox-Gastaut syndrome;
MFG=
middle frontal gyrus;
ROI=
region of interest;
SPM=
Statistical Parametric Mapping

Footnotes

  • Go to Neurology.org/N for full disclosures. Funding information and disclosures deemed relevant by the authors, if any, are provided at the end of the article.

  • ↵* These authors contributed equally to this work.

  • Editorial, page 91

  • Received June 14, 2018.
  • Accepted in final form March 8, 2019.
  • © 2019 American Academy of Neurology
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