| Literature DB >> 30605673 |
Fang Hu1, Jingheng Zhou2, Yanxin Lu2, Lizhao Guan2, Ning-Ning Wei3, Yi-Quan Tang4, KeWei Wang5.
Abstract
The heat shock protein 70 (Hsp70) is upregulated in response to stress and has been implicated as a stress marker in temporal lobe epilepsy (TLE). However, whether Hsp70 plays a pathologic or protective role in TLE remains unclear. Here we report a deleterious role of Hsp70 in kainic acid (KA)-induced seizures. Hsp70 expression is upregulated in a KA model of TLE, and silencing or inhibition of Hsp70 suppresses neuronal hyperexcitability and attenuates acute or chronic epilepsy by enhancing A-type potassium current in hippocampal neurons. Hsp70 upregulation leads to proteosomal degradation of Kv4-KChIP4a channel complexes primarily encoding neuronal A-type current. Furthermore, Hsp70 directly binds to the N terminus of auxiliary KChIP4a and targets Kv4-KChIP4a complexes to proteasome. Taken together, our findings reveal a role of Hsp70 in the pathogenesis of epilepsy through degradation of Kv4-KChIP4a complexes, and pharmacological inhibition of Hsp70 may represent therapeutic potential for epilepsy or hyperexcitability-related neurological disorders.Entities:
Keywords: A-type current; Hsp70; KChIP4a; Kv4; epilepsy; hyperexcitability; kainic acid; seizures; spontaneous recurrent seizures; status epilepticus
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Year: 2019 PMID: 30605673 DOI: 10.1016/j.celrep.2018.12.032
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423