Glial immune-related pathways mediate effects of closed head traumatic brain injury on behavior and lethality in Drosophila.
Bart van AlphenSamuel StewartMarta IwanaszkoFangke XuKeyin LiSydney RozenfeldAnujaianthi RamakrishnanTaichi Q ItohShiju SZuoheng QinBridget C LearRavi AlladaPublished in: PLoS biology (2022)
In traumatic brain injury (TBI), the initial injury phase is followed by a secondary phase that contributes to neurodegeneration, yet the mechanisms leading to neuropathology in vivo remain to be elucidated. To address this question, we developed a Drosophila head-specific model for TBI termed Drosophila Closed Head Injury (dCHI), where well-controlled, nonpenetrating strikes are delivered to the head of unanesthetized flies. This assay recapitulates many TBI phenotypes, including increased mortality, impaired motor control, fragmented sleep, and increased neuronal cell death. TBI results in significant changes in the transcriptome, including up-regulation of genes encoding antimicrobial peptides (AMPs). To test the in vivo functional role of these changes, we examined TBI-dependent behavior and lethality in mutants of the master immune regulator NF-κB, important for AMP induction, and found that while sleep and motor function effects were reduced, lethality effects were enhanced. Similarly, loss of most AMP classes also renders flies susceptible to lethal TBI effects. These studies validate a new Drosophila TBI model and identify immune pathways as in vivo mediators of TBI effects.
Keyphrases
- traumatic brain injury
- severe traumatic brain injury
- cell death
- mild traumatic brain injury
- physical activity
- signaling pathway
- optic nerve
- type diabetes
- coronary artery disease
- spinal cord injury
- cardiovascular events
- cell proliferation
- depressive symptoms
- high throughput
- inflammatory response
- spinal cord
- genome wide identification