| Literature DB >> 26044087 |
Michele Mishto1, Muhammad L Raza2, Dario de Biase3, Teresa Ravizza4, Francesco Vasuri5, Morena Martucci3, Christin Keller6, Elena Bellavista3, Tonia J Buchholz7, Peter M Kloetzel6, Annalisa Pession8, Annamaria Vezzani4, Uwe Heinemann2.
Abstract
The proteasome is the core of the ubiquitin-proteasome system and is involved in synaptic protein metabolism. The incorporation of three inducible immuno-subunits into the proteasome results in the generation of the so-called immunoproteasome, which is endowed of pathophysiological functions related to immunity and inflammation. In healthy human brain, the expression of the key catalytic β5i subunit of the immunoproteasome is almost absent, while it is induced in the epileptogenic foci surgically resected from patients with pharmaco-resistant seizures, including temporal lobe epilepsy. We show here that the β5i immuno-subunit is induced in experimental epilepsy, and its selective pharmacological inhibition significantly prevents, or delays, 4-aminopyridine-induced seizure-like events in acute rat hippocampal/entorhinal cortex slices. These effects are stronger in slices from epileptic vs normal rats, likely due to the more prominent β5i subunit expression in neurons and glia cells of diseased tissue. β5i subunit is transcriptionally induced in epileptogenic tissue likely by Toll-like receptor 4 signaling activation, and independently on promoter methylation. The recent availability of selective β5i subunit inhibitors opens up novel therapeutic opportunities for seizure inhibition in drug-resistant epilepsies.Entities:
Keywords: Neuroinflammation; Pharmaco-resistant seizures; Pilocarpine; Proteasome inhibitors
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Year: 2015 PMID: 26044087 DOI: 10.1016/j.bbi.2015.05.007
Source DB: PubMed Journal: Brain Behav Immun ISSN: 0889-1591 Impact factor: 7.217