Microdysgenesis in temporal lobe epilepsy: A quantitative and immunohistochemical study of white matter neurones

doi:10.1093/brain/124.11.2299

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Brain, Vol. 124, No. 11, 2299-2309, November 2001
© 2001 Oxford University Press

Microdysgenesis in temporal lobe epilepsy

A quantitative and immunohistochemical study of white matter neurones

Maria Thom¹, Sanjay Sisodiya², William Harkness³ and Francesco Scaravilli¹

¹ Departments of Neuropathology, ² Neurology and ³ Neurosurgery, Institute of Neurology, University College London, Queen Square, London WC1N 3BG, UK

Correspondence to: M. Thom, Department of Neuropathology, Institute of Neurology, Queen Square, London, WC1N 3BG, UK E-mail: M.Thom{at}ion.ucl.ac.uk

Microdysgenesis is a microscopic cortical malformation consideredto act as a substrate for seizures in some patients with generalizedepilepsy. It is also recognized to involve the temporal lobein a proportion of patients with intractable temporal lobe epilepsy,but the incidence of this abnormality, its relationship to mesialtemporal lobe sclerosis and relevance to epileptogenesis remainunknown. This is partly due to a lack of well-defined quantitativepathological diagnostic criteria. To begin to address theseissues, we have carried out a rigorous quantitative analysis,using three-dimensional cell counting methods, of several componentsof microdysgenesis in temporal lobectomy specimens. White matter,cortical and layer I neuronal densities (NDs) were measuredusing immunohistochemistry for the neuronal markers neuronalnuclear antigen and calbindin D-28-K. Patients with a seizure-freeoutcome (Class I) showed significantly more microdysgeneticfeatures including higher white matter ND (P < 0.05), particularlyof small (<10 µm diameter) neurones (P < 0.01),higher layer I ND (P < 0.05) and increased numbers of Cajal–Retzius-likecalbindin-positive neurones (P < 0.05). We also demonstratedthat white matter ND was independent of the degree of temporallobe gliosis as assessed by quantitation of glial fibrillaryacidic protein-immunoreactive cells. These findings suggestthat microdysgenesis may be a significant lesion in temporallobe epilepsy in terms of post-surgical prognosis.

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