Abstracts

This is a Late Breaking abstract

Rationale: Mutations of the sodium-activated potassium channel K_Na1.1, has been reported in multiple epileptic disorders. However, whether K_Na1.1 channel is involved in epileptogenesis after traumatic brain injury (TBI) remains unknown.

Methods: Firstly, we used EEG and patch-clamp recordings to examine spontaneous seizure activity, seizure susceptibility and neuronal excitability after TBI. Meanwhile, we explored the changes of K_Na1.1 channel following TBI. To further determine the role of K_Na1.1 channel after TBI, we built TBI models using the null mutant kcnt1^−/− mice and compared seizure activity with those on wild-type (WT) mice. Finally, we investigated whether the K_Na1.1 channel was regulated by the activated MAPK pathway after TBI in in vitro experiment.

Results: We found enhanced seizure susceptibility and increased neuronal excitability in the moderate TBI model. In addition, increased neuronal expression of K_Na1.1 channel around the lesion was also observed following TBI. Compared to WT littermates, kcnt1^−/− mice displayed decreased seizure susceptibility to the pentylenetetrazole (PTZ) after TBI. Moreover, we found that the p38 MAPK pathway after TBI upregulated the K_Na1.1 channel.

Conclusions: Taken together, this study suggests that enhanced K_Na1.1 activated by inflammatory response contributes to seizure susceptibility in the moderate TBI model and provides a potential therapeutic target on the post-traumatic epilepsy.

Funding: This work was supported by the National Natural Science Foundation of China (81870935, J.W.), the startup fund from Capital Medical University Advanced Innovation Center for Human Brain Protection (20181101, J.W.), and the Natural Science Foundation of Beijing (7214224, M.J.).