TPL2 kinase activity regulates microglial inflammatory responses and promotes neurodegeneration in tauopathy mice.
Yuanyuan WangTiffany WuMing-Chi TsaiMitchell G RezzonicoAlyaa M Abdel-HaleemLuke XieVineela D GandhamHai NguKimberly StarkCaspar GlockDaqi XuOded ForemanBrad A FriedmanMorgan ShengJesse E HansonPublished in: eLife (2023)
Tumor progression locus 2 (TPL2) (MAP3K8) is a central signaling node in the inflammatory response of peripheral immune cells. We find that TPL2 kinase activity modulates microglial cytokine release and is required for microglia-mediated neuron death in vitro. In acute in vivo neuroinflammation settings, TPL2 kinase activity regulates microglia activation states and brain cytokine levels. In a tauopathy model of chronic neurodegeneration, loss of TPL2 kinase activity reduces neuroinflammation and rescues synapse loss, brain volume loss, and behavioral deficits. Single-cell RNA sequencing analysis indicates that protection in the tauopathy model was associated with reductions in activated microglia subpopulations as well as infiltrating peripheral immune cells. Overall, using various models, we find that TPL2 kinase activity can promote multiple harmful consequences of microglial activation in the brain including cytokine release, iNOS (inducible nitric oxide synthase) induction, astrocyte activation, and immune cell infiltration. Consequently, inhibiting TPL2 kinase activity could represent a potential therapeutic strategy in neurodegenerative conditions.
Keyphrases
- inflammatory response
- lipopolysaccharide induced
- lps induced
- single cell
- protein kinase
- nitric oxide synthase
- neuropathic pain
- traumatic brain injury
- tyrosine kinase
- type diabetes
- nitric oxide
- white matter
- resting state
- poor prognosis
- lymph node
- metabolic syndrome
- cerebral ischemia
- high throughput
- brain injury
- liver failure
- spinal cord injury
- mouse model
- functional connectivity
- drug induced