Common Ictal and Interictal Perfusion Patterns: A Window into the Epileptogenic Network and SUDEP Mechanism in Drug-Resistant Focal Epilepsy

Author:

Chacón Lilia M. Morales1ORCID,García Lidice Galan2,García-Ramón Karla Batista1ORCID,Báez Martin Margarita Minou1,Bosch-Bayard Jorge3,Alfonso Maydelis Alfonso1ORCID,Batista Sheyla Berrillo1,Bermudez Tania de la Paz1ORCID,González Judith González1,Coroneaux Abel Sánchez1,Ruiz Ángel Águila1,Roque Marlene Perera1,Matamoro Leysi Murada1

Affiliation:

1. Clinical Neurophysiology Department, International Center for Neurological Restoration. Avenida 25 e/ 158 y 160 No 15805, Habana, Cuba

2. Cuban Epilepsy Program, Cuban Neuroscience Center, Havana, Cuba

3. McGill Centre for Integrative Neuroscience, Ludmer Centre for Neuroinformatics and Mental health, Montreal Neurological Institute, Montreal, PC H3A 0G4, Canada

Abstract

Background: Focal epilepsies have been described as network disease. Noninvasive investigative techniques have been used to characterize epileptogenic networks. Objetive: To describe ictal and interictal cortical and subcortical perfusion patterns using single photon emission computed tomography (SPECT), in patients with drug-resistant epilepsy (DRE). Methods: Thirty-five interictal- ictal SPECT scans were obtained from 15 patients with DRE. A methodology was developed to get a relative perfusion index (PI) of 74 cortical and sub-cortical brain structures. K-means algorithm together with a modified v-fold cross-validation were used to identify the two regions of interest (ROI's) that represent hypoperfused and hyperperfused areas. Results: In common with the individual analysis, the statistical analysis evidenced that the hyperperfusion ROIs resulting from group analysis during interictal, and ictal involved mainly the cingulate gyrus, cuneus, the lingual gyrus, gyrus rectus as well as the putamen. ROIs hypoperfused included the red nucleus, the substantia nigra, and the medulla. The medians of the group analysis of the hypoperfusion and hyperperfusion ROIs were 0.601-0.565 and 1,133 - 1,119 for the ictal and interictal states, correspondingly. A group of mostly cortical structures involved in the hyperperfused ROIs in both interictal and ictal states showed no change or negative change in the transition from interictal to ictal state (mean change of -0.002). On the other hand, the brain stem, basal ganglia, red nucleus, and thalamus revealed a mean global change of 0.19, indicating a mild increase in the PI. However, some of these structures (red nucleus, substantia nigra, and medulla oblongata) remained hypoperfused during the interictal to ictal transition. Conclusion: The methodology employed made it possible to identify common cortical and subcortical perfusion patterns not directly linked to epileptogenicity, but open a window for the epileptogenic network and sudden unexpected death (SUDEP) mechanism in DRE .

Publisher

Bentham Science Publishers Ltd.

Subject

Drug Discovery,Pharmacology

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