Multimodal computational neocortical anatomy in pediatric hippocampal sclerosis

Autor:	Seok-Jun Hong, Torsten Baldeweg, Martin Tisdall, Neda Bernasconi, J. Helen Cross, David W. Carmichael, Andrea Bernasconi, Thomas S. Jacques, Roxana Gunny, Boris C. Bernhardt, Sophie Adler, Gemma B. Northam, Mallory Blackwood
Rok vydání:	2018
Předmět:	0301 basic medicine Hippocampal sclerosis Neocortex business.industry General Neuroscience Hippocampus Fluid-attenuated inversion recovery Hippocampal formation medicine.disease Hyperintensity Temporal lobe 03 medical and health sciences 030104 developmental biology 0302 clinical medicine Atrophy medicine.anatomical_structure Medicine Neurology (clinical) business Neuroscience Research Articles 030217 neurology & neurosurgery Research Article
Zdroj:	Annals of Clinical and Translational Neurology
ISSN:	2328-9503
DOI:	10.1002/acn3.634
Popis:	Objective In contrast to adult cohorts, neocortical changes in epileptic children with hippocampal damage are not well characterized. Here, we mapped multimodal neocortical markers of epilepsy‐related structural compromise in a pediatric cohort of temporal lobe epilepsy and explored how they relate to clinical factors. Methods We measured cortical thickness, gray–white matter intensity contrast and intracortical FLAIR intensity in 22 patients with hippocampal sclerosis (HS) and 30 controls. Surface‐based linear models assessed between‐group differences in morphological and MR signal intensity markers. Structural integrity of the hippocampus was measured by quantifying atrophy and FLAIR patterns. Linear models were used to evaluate the relationships between hippocampal and neocortical MRI markers and clinical factors. Results In the hippocampus, patients demonstrated ipsilateral atrophy and bilateral FLAIR hyperintensity. In the neocortex, patients showed FLAIR signal hyperintensities and gray–white matter boundary blurring in the ipsilesional mesial and lateral temporal neocortex. In contrast, cortical thinning was minimal and restricted to a small area of the ipsilesional temporal pole. Furthermore, patients with a history of febrile convulsions demonstrated more pronounced FLAIR hyperintensity in the ipsilesional temporal neocortex. Interpretation Pediatric HS patients do not yet demonstrate the widespread cortical thinning present in adult cohorts, which may reflect consequences of a protracted disease process. However, pronounced temporal neocortical FLAIR hyperintensity and blurring of the gray–white matter boundary are already detectable, suggesting that alterations in MR signal intensities may reflect a different underlying pathophysiology that is detectable earlier in the disease and more pervasive in patients with a history of febrile convulsions.
Databáze:	OpenAIRE
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