%0 Journal Article
%T Autoimmune Epilepsy: Some Epilepsy Patients Harbor Autoantibodies to Glutamate Receptors and dsDNA on both Sides of the Blood-brain Barrier, which may Kill Neurons and Decrease in Brain Fluids after Hemispherotomy
%A Yonatan Ganor
%A Hadassa Goldberg-Stern
%A Dina Amrom
%A Tally Lerman-Sagie
%A Vivian I. Teichberg
%A Dori Pelled
%A Anthony H. Futerman
%A Bruria Ben Zeev
%A Michael Freilinger
%A Denis Verheulpen
%A Patrick Van Bogaert
%A Mia Levite
%J Clinical and Developmental Immunology
%D 2004
%I Hindawi Publishing Corporation
%R 10.1080/17402520400001736
%X Purpose: Elucidating the potential contribution of specific autoantibodies (Ab&#39;s) to the etiology and/or pathology of some human epilepsies. Methods: Six epilepsy patients with Rasmussen&#39;s encephalitis (RE) and 71 patients with other epilepsies were tested for Ab&#39;s to the &#8211;B&#8212; peptide (amino acids 372-395) of the glutamate/AMPA subtype 3 receptor (GluR3B peptide), double-stranded DNA (dsDNA), and additional autoimmune disease-associated autoantigens, and for the ability of their serum and cerebrospinal-fluid (CSF) to kill neurons. Results: Elevated anti-GluR3B Ab&#39;s were found in serum and CSF of most RE patients, and in serum of 17/71 (24%) patients with other epilepsies. In two RE patients, anti-GluR3B Ab&#39;s decreased drastically in CSF following functional-hemispherotomy, in association with seizure cessation and neurological improvement. Serum and CSF of two RE patients, and serum of 12/71 (17%) patients with other epilepsies, contained elevated anti-dsDNA Ab&#39;s, the hallmark of systemic-lupus-erythematosus. The sera (but not the CSF) of some RE patients contained also clinically elevated levels of &#8211;classical&#8212; autoimmune Ab&#39;s to glutamic-acid-decarboxylase, cardiolipin, &#946;2-glycoprotein-I and nuclear-antigens SS-A and RNP-70. Sera and CSF of some RE patients caused substantial death of hippocampal neurons. Conclusions: Some epilepsy patients harbor Ab&#39;s to GluR3 and dsDNA on both sides of the blood-brain barrier, and additional autoimmune Ab&#39;s only in serum. Since all these Ab&#39;s may be detrimental to the nervous system and/or peripheral organs, we recommend testing for their presence in epilepsy, and silencing their activity in Ab-positive patients.
%U http://www.hindawi.com/journals/cdi/2004/975378/abs/