4.5 Article

Focal to bilateral tonic-clonic seizures are associated with widespread network abnormality in temporal lobe epilepsy

Journal

EPILEPSIA
Volume 62, Issue 3, Pages 729-741

Publisher

WILEY
DOI: 10.1111/epi.16819

Keywords

connectome; diffusion MRI; drug-resistant epilepsy; network abnormality; node abnormality; secondary generalized seizures

Funding

  1. Medical Research Council [G0802012, MR/M00841X/1]
  2. Wellcome Trust [105617/Z/14/Z, 208940/Z/17/Z, 210109/Z/18/Z]
  3. Faculty of Medical Sciences, Newcastle University
  4. UCLH Biomedical Research Centre
  5. Wellcome Trust [105617/Z/14/Z, 210109/Z/18/Z] Funding Source: Wellcome Trust
  6. EPSRC [EP/M020533/1] Funding Source: UKRI
  7. MRC [MR/M00841X/1, G0802012] Funding Source: UKRI
  8. Engineering and Physical Sciences Research Council [EP/M020533/1] Funding Source: researchfish

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The study found that in patients with TLE and FBTCS, the whole-brain structural network is altered to a greater extent and more widespread. These abnormal networks may serve as an underlying structural basis or consequence of the observed greater seizure spread in FBTCS.
Objective Our objective was to identify whether the whole-brain structural network alterations in patients with temporal lobe epilepsy (TLE) and focal to bilateral tonic-clonic seizures (FBTCS) differ from alterations in patients without FBTCS. Methods We dichotomized a cohort of 83 drug-resistant patients with TLE into those with and without FBTCS and compared each group to 29 healthy controls. For each subject, we used diffusion-weighted magnetic resonance imaging to construct whole-brain structural networks. First, we measured the extent of alterations by performing FBTCS-negative (FBTCS-) versus control and FBTCS-positive (FBTCS+) versus control comparisons, thereby delineating altered subnetworks of the whole-brain structural network. Second, by standardizing each patient's networks using control networks, we measured the subject-specific abnormality at every brain region in the network, thereby quantifying the spatial localization and the amount of abnormality in every patient. Results Both FBTCS+ and FBTCS- patient groups had altered subnetworks with reduced fractional anisotropy and increased mean diffusivity compared to controls. The altered subnetwork in FBTCS+ patients was more widespread than in FBTCS- patients (441 connections altered at t > 3, p t > 3, p = .01 in FBTCS-). Significantly greater abnormalities-aggregated over the entire brain network as well as assessed at the resolution of individual brain areas-were present in FBTCS+ patients (p < .001, d = .82, 95% confidence interval = .32-1.3). In contrast, the fewer abnormalities present in FBTCS- patients were mainly localized to the temporal and frontal areas. Significance The whole-brain structural network is altered to a greater and more widespread extent in patients with TLE and FBTCS. We suggest that these abnormal networks may serve as an underlying structural basis or consequence of the greater seizure spread observed in FBTCS.

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