An analysis of clinical seizure patterns and their localizing value in frontal and temporal lobe epilepsies

doi:10.1093/brain/119.1.17

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Brain, Vol. 119, No. 1, 17-40, 1996
© 1996 Oxford University Press

research-article

An analysis of clinical seizure patterns and their localizing value in frontal and temporal lobe epilepsies

M. Manford¹^,, D. R. Fish² and S. D. Shorvon²

¹Wessex Neurological Centre, Southampton General Hospital ²Epilepsy Research Group, Institute of Neurology London, UK

Correspondence to: Dr M. Manford, Wessex Neurological Centre, Southampton General Hospital, Tremona Road, Southampton SO16 6YD, UK

The differentiation of frontal lobe epilepsy (FLE) and temporallobe epilepsy (TLE) is a clinical problem of major theoreticaland practical importance. Current electroclinical classificationis based on retrospective studies of highly selected patients.When applied to the presurgical evaluation of patients, it haspoor specificity. The current study adopts a different and prospectiveapproach to the analysis of ictal clinical manifestations andtheir value in differentiating FLE and TLE. Two hundred andfifty-two patients with partial epilepsy were selected accordingto criteria of focal abnormality on imaging, ictal EEG or interictalEEG or highly focal clinical pattern. A witnessed seizure descriptionwas obtained for each of their habitual seizures and the sequenceof manifestations encoded and entered into a statistical clusteranalysis to form a clinical classification of the 352 seizuresidentified, which comprised 14 clinical groups. Neuroimagingabnormalities were measured, using a template technique, andgraded 0–3 according to extent of involvement of eachregion in the lesion, using standard anatomical divisions. A ${chi}$ ² analysis of lesion location against seizure type was performedto assess the strength of association of seizure types withspecific cerebral regions. The distribution of interictal EEGspikes and ictal EEG onsets were assessed qualitatively. Anindependent analysis was also performed, comparing clinicalseizure manifestations associated with lesions restricted toeither frontal or temporal lobes. Of the 14 clinical groups,four were predominantly related to temporal lobe abnormalites:fear/olfactory/gustatory; absence with no focal symptoms; experientialand visual. Within these groups, 45 out of 58 lesional casesinvolved the temporal lobes (P << 0.001). A minority ofseizures in these groups were associated with frontal lesionsand these seizures were significantly more likely to evolveto version/posturing, without an intervening absence phase,than the temporal cases (P < 0.001). Two groups were relatedto perirolandic abnormalities; somatosensory and Jacksonianclonic with 22 out of 24 lesional cases involving this region(P < 0.001). Two other groups were related to the frontallobes; version/posturing and motor agitation. Early focal tonicactivity or head turning were associated with lateral premotorlesions (P < 0.001) and ictal and interictal EEG showed strongfrontal predominance. Seizures characterized by general motoragitation were associated with lesions of the orbitofrontal(eight out of 13 cases) and frontopolar (six out of 13 cases)cortices (P < 0.001). Location of interictal EEG spikes andictal EEG onsets were generally consistent with lesion sitesand where there were discrepancies, EEG localization tendedto be more diffuse than lesion localization, rather than franklydiscordant. Analysis of manifestations associated with purefrontal and pure temporal lesions supported the results of thecluster analysis and also showed a significant association oforo-alimentary automatisms with temporal lobe abnormalities.There were no consistent differences between groups with differentlocalizations in terms of seizure frequency or other characteristicsof seizure timing, although very high seizure frequencies wereseen more often in association with frontal lesions. Only onecombination of different seizure types in the same patient occurredwith statistical significance: absence and generalized motorseizures and pseudo generalized epilepsy. The results of thisstudy suggest that relatively few seizures can be localizedreliably on clinical grounds and that even in those seizuretypes where there is a statistically significant associationwith specific cortical areas, an important minority do not sharethe same associations. Analysis of the seizure evolution aswell as initial symptoms may be of value in localizing somecases, but even here wide variation occurs. These findings leadus to question the value of classifiying partial epilepsy usingelectroclinical criteria, particularly in trying to infer anatomicallocalization. Possible mechanisms for blurring of the distinctionsof clinical seizure types are discussed.

epilepsy; classification; temporal lobe; frontal lobe; lesion

Received June 15, 1995. Accepted August 10, 1995.

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