P2X7R antagonism suppresses long-lasting brain hyperexcitability following traumatic brain injury in mice.

Mariana Alves,Laura De Diego-Garcia,Gloria Vegliante,Oscar Moreno,Beatriz Gil,Pedro Ramos-Cabrer,Meghma Mitra,Ana Fernandez Martin,Aida Menéndez-Méndez,Yitao Wang,Nathan Ryzewski Strogulski,Meng-Juan Sun,Ciara Melia,Giorgia Conte,Sandra Plaza-García,Igor Khalin,Xinchen Teng,Nikolaus Plesnila,Bert Klebl,Klaus Dinkel,Michael Hamacher,Anindya Bhattacharya,Marc Ceusters,James Palmer,David J Loane,Jordi Llop,David C Henshall,Tobias Engel

doi:10.7150/thno.97254

Mariana Alves, Laura De Diego-Garcia + Show 26 more

https://doi.org/10.7150/thno.97254

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Journal: Theranostics

Publication Date: Jan 1, 2025

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Purpose: Post-traumatic epilepsy (PTE) is one of the most common life-quality reducing consequences of traumatic brain injury (TBI). However, to date there are no pharmacological approaches to predict or to prevent the development of PTE. The P2X7 receptor (P2X7R) is a cationic ATP-dependent membrane channel that is expressed throughout the brain. While increasing evidence suggests a role for the P2X7R during seizures and epilepsy, it is unclear if changes in P2X7R expression can predict TBI-induced epilepsy development, and whether P2X7R antagonism can protect against long-lasting brain hyperexcitability caused by TBI. Methods: TBI was induced in adult male mice using the controlled cortical impact model (CCI). To test the anti-epileptogenic effects of P2X7R antagonism, mice were treated with brain-penetrant P2X7R antagonists JNJ-54175446 (30 mg/kg) or AFC-5128 (30 mg/kg) for 7 days post-CCI. The cell-type specific effects of P2X7Rs on TBI-induced hyperexcitability were analyzed in mice lacking exon 2 of the P2rx7 gene selectively in microglia (P2rx7:Cx3cr1-Cre). Static positron emission tomography (PET) via an intravenous injection of the P2X7R radioligand 18F-JNJ-64413739 and magnetic resonance imaging (MRI) were conducted twice during the first- and third-week post-injury. Results: Following TBI, while there were no obvious changes in P2X7R protein levels in the ipsilateral hippocampus post-injury, there was a delayed increase in P2X7R protein levels in the ipsilateral cortex at 3 months post-injury. Treatment with P2X7R antagonists shortly after TBI reduced long-lasting brain hyperexcitability, reduced cortical contusion volume, and normalized injury-induced hyperactivity to control sham-levels at 3 weeks post-TBI. Notably, mice lacking P2rx7 in microglia had an increased seizure threshold after TBI, suggesting that P2X7R contributed to brain hyperexcitability via its effects on microglia. Finally, P2X7R radioligand uptake after TBI correlated with seizure threshold at 3 weeks post-injury. Conclusions: Our results demonstrate the antiepileptogenic potential of P2X7R antagonism to prevent TBI-induced epilepsy and indicate that P2X7R-based PET imaging may be a useful diagnostic tool to identify people at risk of developing PTE.

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