MRI-negative PET-positive temporal lobe epilepsy: a distinct surgically remediable syndrome

doi:10.1093/brain/awh257

Brain Advance Access originally published online on July 28, 2004
Brain 2004 127(10):2276-2285; doi:10.1093/brain/awh257

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MRI-negative PET-positive temporal lobe epilepsy: a distinct surgically remediable syndrome

R. P. Carne¹^,3^,4, T. J. O'Brien⁴^,6, C. J. Kilpatrick⁴^,6, L. R. MacGregor⁴^,7, R. J. Hicks², M. A. Murphy¹^,3^,5, S. C. Bowden⁸, A. H. Kaye⁴^,6 and M. J. Cook¹^,3^,5

¹ Victorian Epilepsy Centre, St Vincent's Hospital, ² PET Centre, The Peter MacCallum Cancer Institute, ³ Departments of Neurology and Neurosurgery, St. Vincent's Hospital, ⁴ The Royal Melbourne Hospital, The University of Melbourne and Departments of Medicine and Surgery, ⁵ St. Vincent's Hospital and ⁶ The Royal Melbourne Hospital, ⁷ Department of Clinical Epidemiology and Biostatistics, The Royal Melbourne Hospital, ⁸ Department of Psychology, The University of Melbourne, Victoria, Australia

Correspondence to: Dr Ross Carne, Department of Clinical Neurosciences, Geelong Hospital, Level 2, Kardinia House, Bellerine St, Geelong, Victoria 3220, Australia E-mail: carnero{at}svhm.org.au

Most patients with non-lesional temporal lobe epilepsy (NLTLE)will have the findings of hippocampal sclerosis (HS) on a highresolution MRI. However, a significant minority of patientswith NLTLE and electroclinically well-lateralized temporal lobeseizures have no evidence of HS on MRI. Many of these patientshave concordant hypometabolism on fluorodeoxyglucose-PET ([¹⁸F]FDG-PET).The pathophysiological basis of this latter group remains uncertain.We aimed to determine whether NLTLE without HS on MRI representsa variant of or a different clinicopathological syndrome fromthat of NLTLE with HS on MRI. The clinical, EEG, [¹⁸F]FDG-PET,histopathological and surgical outcomes of 30 consecutive NLTLEpatients with well-lateralized EEG but without HS on MRI (HS–veTLE) were compared with 30 consecutive age- and sex-matchedNLTLE patients with well-lateralized EEG with HS on MRI (HS+veTLE). Both the HS+ve TLE group and the HS–ve TLE patientshad a high degree of [¹⁸F]FDG-PET concordant lateralization(26 out of 30 HS–ve TLE versus 27 out of 27 HS+ve TLE).HS–ve TLE patients had more widespread hypometabolismon [¹⁸F]FDG-PET by blinded visual analysis [odds ratio (OR =+ ${infty}$ (2.51, –), P = 0.001]. The HS–ve TLE group lessfrequently had a history of febrile convulsions [OR = 0.077(0.002–0.512), P = 0.002], more commonly had a delta rhythmat ictal onset [OR = 3.67 (0.97–20.47), P = 0.057], andless frequently had histopathological evidence of HS [OR = 0(0–0.85), P = 0.031]. There was no significant differencein surgical outcome despite half of those without HS havinga hippocampal-sparing procedure. Based on the findings outlined,HS–ve PET-positive TLE may be a surgically remediablesyndrome distinct from HS+ve TLE, with a pathophysiologicalbasis that primarily involves lateral temporal neocortical ratherthan mesial temporal structures.

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