Synchrotron-generated microbeams induce hippocampal transections in rats

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作者
Erminia Fardone
Benoît Pouyatos
Elke Bräuer-Krisch
Stefan Bartzsch
Hervè Mathieu
Herwig Requardt
Domenico Bucci
Giacomo Barbone
Paola Coan
Giuseppe Battaglia
Geraldine Le Duc
Alberto Bravin
Pantaleo Romanelli
机构
[1] European Synchrotron Radiation Facility (ESRF),Department of Radiation Oncology
[2] Grenoble Institut des Neurosciences,Department of Physics
[3] Inserm U836,Department of Clinical Radiology
[4] Université Joseph Fourier,Department of Biological Science and Program in Neuroscience
[5] Klinikum rechts der Isar,undefined
[6] Technical University of Munich,undefined
[7] The Institute of Cancer Research,undefined
[8] I.R.C.C.S. Neuromed,undefined
[9] Ludwig Maximilians University,undefined
[10] Ludwig Maximilians University,undefined
[11] Brain Radiosurgery,undefined
[12] Cyberknife Center,undefined
[13] Centro Diagnostico Italiano (CDI),undefined
[14] Florida State University,undefined
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摘要
Synchrotron-generated microplanar beams (microbeams) provide the most stereo-selective irradiation modality known today. This novel irradiation modality has been shown to control seizures originating from eloquent cortex causing no neurological deficit in experimental animals. To test the hypothesis that application of microbeams in the hippocampus, the most common source of refractory seizures, is safe and does not induce severe side effects, we used microbeams to induce transections to the hippocampus of healthy rats. An array of parallel microbeams carrying an incident dose of 600 Gy was delivered to the rat hippocampus. Immunohistochemistry of phosphorylated γ-H2AX showed cell death along the microbeam irradiation paths in rats 48 hours after irradiation. No evident behavioral or neurological deficits were observed during the 3-month period of observation. MR imaging showed no signs of radio-induced edema or radionecrosis 3 months after irradiation. Histological analysis showed a very well preserved hippocampal cytoarchitecture and confirmed the presence of clear-cut microscopic transections across the hippocampus. These data support the use of synchrotron-generated microbeams as a novel tool to slice the hippocampus of living rats in a minimally invasive way, providing (i) a novel experimental model to study hippocampal function and (ii) a new treatment tool for patients affected by refractory epilepsy induced by mesial temporal sclerosis.
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