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Vol. 57 No. 5, May 2000 TABLE OF CONTENTS
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Stereotaxic Injection of IgG From Patients With Alzheimer Disease Initiates Injury of Cholinergic Neurons of the Basal Forebrain

József I. Engelhardt, MD, PhD; Wei-Dong Le, MD, PhD; László Siklós, PhD; Izabella Obál, MD; Krisztina Boda, PhD; Stanley H. Appel, MD

Arch Neurol. 2000;57:681-686.

Context  The participation of an immune/inflammatory process in the pathomechanism of sporadic Alzheimer disease (AD) has been suggested by evidence for activated microglia and the potential therapeutic benefit of anti-inflammatory medication.

Objective  To define a possible role for IgG in the immune/inflammatory process of AD in humans, we assayed the ability of IgG samples from patients with AD to target the injury to cholinergic neurons in rat basal forebrain in vivo.

Design  IgG purified from the serum or plasma from patients with AD and patients with other neurological disease who were used as control (DC) patients was injected stereotaxically into the medial septum of adult rats. Four weeks later coronal sections of the whole medial septum–diagonal bands of Broca region were immunostained for choline acetyltransferase (ChAT) to identify cholinergic neuronal cells.

Setting  University medical centers.

Patients  Blood samples were collected from 8 patients with probable and definite AD and from 6 age-matched DC patients.

Main Outcome Measure  Detection of changes in the number of ChAT immunopositive cell profiles in sections and statistical evaluation.

Results  Four weeks after the injections, IgG samples from patients with AD significantly reduced the number of ChAT-immunostained cell profiles in the whole medial septum–diagonal bands of Broca region compared with IgGs from DC patients. Neither DC IgGs nor saline solution significantly decreased the number of ChAT-immunopositive neuronal cell profiles.

Conclusion  Data document that IgG from patients with AD can target a stereotaxically induced immune/inflammatory injury to cholinergic neurons in the rat basal forebrain in vivo.


From the Department of Neurology, Baylor College of Medicine, Houston, Tex (Drs Engelhardt, Le, Siklós, and Appel); and the Departments of Neurology and Psychiatry (Drs Engelhardt and Obál) and Medical Informatics (Dr Boda), Albert Szent-Györgyi Medical University, and the Institute of Biophysics, Biological Research Center of the Hungarian Academy of Sciences (Dr Siklós), Szeged, Hungary.


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