Seizures are a druggable mechanistic link between TBI and subsequent tauopathy.
Hadeel AlyenbaawiRichard KanyoLaszlo F LocskaiRazieh Kamali-JamilMichèle G DuValQing BaiHolger WilleEdward A BurtonW Ted AllisonPublished in: eLife (2021)
Traumatic brain injury (TBI) is a prominent risk factor for dementias including tauopathies like chronic traumatic encephalopathy (CTE). The mechanisms that promote prion-like spreading of Tau aggregates after TBI are not fully understood, in part due to lack of tractable animal models. Here, we test the putative role of seizures in promoting the spread of tauopathy. We introduce 'tauopathy reporter' zebrafish expressing a genetically encoded fluorescent Tau biosensor that reliably reports accumulation of human Tau species when seeded via intraventricular brain injections. Subjecting zebrafish larvae to a novel TBI paradigm produced various TBI features including cell death, post-traumatic seizures, and Tau inclusions. Bath application of dynamin inhibitors or anticonvulsant drugs rescued TBI-induced tauopathy and cell death. These data suggest a role for seizure activity in the prion-like seeding and spreading of tauopathy following TBI. Further work is warranted regarding anti-convulsants that dampen post-traumatic seizures as a route to moderating subsequent tauopathy.
Keyphrases
- traumatic brain injury
- cell death
- severe traumatic brain injury
- mild traumatic brain injury
- cerebrospinal fluid
- spinal cord injury
- quantum dots
- endothelial cells
- temporal lobe epilepsy
- social support
- emergency department
- sensitive detection
- crispr cas
- artificial intelligence
- high glucose
- multiple sclerosis
- label free
- resting state
- big data
- cell cycle arrest
- depressive symptoms
- functional connectivity
- drug induced
- blood brain barrier
- machine learning
- induced pluripotent stem cells
- aedes aegypti
- adverse drug