Electron microscopy of tissue adherent to explanted electrodes in dystonia and Parkinson's disease

doi:10.1093/brain/awh292

Brain Advance Access published online on August 25, 2004
Brain, doi:10.1093/brain/awh292
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Received April 26, 2004
Revised July 19, 2004
Accepted July 20, 2004

Article

Electron microscopy of tissue adherent to explanted electrodes in dystonia and Parkinson's disease

J. Moss ¹, T. Ryder ¹, T. Z. Aziz ², M. B. Graeber ³, P. G. Bain ²^*

¹ Electron Microscopy Unit, Department of Histopathology, Charing Cross Hospital, Hammersmith Hospitals NHS Trust, London
² Department of Clinical Neurosciences, Division of Neuroscience and Psychological Medicine, Charing Cross Campus, Imperial College London, London, UK
³ Department of Neuropathology, Division of Neuroscience and Psychological Medicine, Charing Cross Campus, Imperial College London, London, UK

^* To whom correspondence should be addressed. E-mail: p.bain{at}ic.ac.uk.

Abstract

Summary Deep brain stimulation (DBS) is used to treat a varietyof severe medically intractable movement disorders, includingParkinson's disease, tremor and dystonia. There have been fewstudies examining the effect of chronic DBS on the brains ofParkinson's disease patients. Most of these post mortem studiesconcluded that chronic DBS caused mild gliosis around the leadtrack and did not damage brain tissue. There have been no similarhistopathological studies on brains from dystonic patients whohave undergone DBS. In this study, our objective was to discoverwhether tissue would be attached to DBS electrodes removed frompatients for routine clinical reasons. We hoped that by examiningexplanted DBS electrodes using scanning (SEM) and/or transmission(TEM) electron microscopy we might visualize any attached tissueand thus understand the electrode-human brain tissue interactionmore accurately. Initially, SEM was performed on one controlDBS electrode that had not been implanted. Then 21 (one subthalamicnucleus and 20 globus pallidus internus) explanted DBS electrodeswere prepared, after fixation in 3% glutaraldehyde, for SEM(n = 9) or TEM (n = 10), or both (n = 2), according to departmentalprotocol. The electrodes were sourced from two patients withParkinson's disease, one with myoclonic dystonia, two with cervicaldystonia and five with primary generalized dystonia, and hadbeen in situ for 11 and 31 months (Parkinson's disease), 16months (myoclonic dystonia), 14 and 24 months (cervical dystonia)and 3-24 months (primary generalized dystonia). Our resultsshowed that a foreign body multinucleate giant cell-type reactionwas present in all TEM samples and in SEM samples, prewashedto remove surface blood and fibrin, regardless of the diagnosis.Some of the giant cells were >100 µm in diameter andmight have originated from either fusion of parenchymal microglia,resident perivascular macrophage precursors and/or monocytes/macrophagesinvading from the blood stream. The presence of mononuclearmacrophages containing lysosomes and sometimes having conspicuousfilopodia was detected by TEM. Both types of cell containedhighly electron-dense inclusions, which probably represent phagocytosedmaterial. Similar material, the exact nature of which is unknown,was also seen in the vicinity of these cells. This reactionwas present irrespective of the duration of implantation andmay be a response to the polyurethane component of the electrodes'surface coat. These findings may be relevant to our understandingof the time course of the clinical response to DBS in Parkinson'sdisease and various forms of dystonia, as well as contributingto the design characteristics of future DBS electrodes.

Keywords: deep brain stimulation; dystonia; electron microscopy; giant cell reaction; Parkinson's disease.

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