p17/C18-ceramide-mediated mitophagy is an endogenous neuroprotective response in preclinical and clinical brain injury.
Eda KarakayaNatalia OleinikJazlyn EdwardsJensen TomberlinRandy Bent BarkerBurak BerberMaria EricssonHabeeb AlsudaniAdviye ErgulSemir BeyazJohn J LemastersBesim OgretmenOnder AlbayramPublished in: PNAS nexus (2024)
Repeat concussions (or repetitive mild traumatic brain injury [rmTBI]) are complex pathological processes consisting of a primary insult and long-term secondary complications and are also a prerequisite for chronic traumatic encephalopathy (CTE). Recent evidence implies a significant role of autophagy-mediated dysfunctional mitochondrial clearance, mitophagy, in the cascade of secondary deleterious events resulting from TBI. C18-ceramide, a bioactive sphingolipid produced in response to cell stress and damage, and its synthesizing enzyme (CerS1) are precursors to selective stress-mediated mitophagy. A transporter, p17, mediates the trafficking of CerS1, induces C18-ceramide synthesis in the mitochondrial membrane, and acts as an elimination signal in cell survival. Whether p17-mediated mitophagy occurs in the brain and plays a causal role in mitochondrial quality control in secondary disease development after rmTBI are unknown. Using a novel repetitive less-than-mild TBI (rlmTBI) injury paradigm, ablation of mitochondrial p17/C18-ceramide trafficking in p17 knockout (KO) mice results in a loss of C18-ceramide-induced mitophagy, which contributes to susceptibility and recovery from long-term secondary complications associated with rlmTBI. Using a ceramide analog with lipid-selenium conjugate drug, LCL768 restored mitophagy and reduced long-term secondary complications, improving cognitive deficits in rlmTBI-induced p17KO mice. We obtained a significant reduction of p17 expression and a considerable decrease of CerS1 and C18-ceramide levels in cortical mitochondria of CTE human brains compared with age-matched control brains. These data demonstrated that p17/C18-ceramide trafficking is an endogenous neuroprotective mitochondrial stress response following rlmTBI, thus suggesting a novel prospective strategy to interrupt the CTE consequences of concussive TBI.
Keyphrases
- mild traumatic brain injury
- oxidative stress
- brain injury
- traumatic brain injury
- diabetic rats
- nlrp inflammasome
- cerebral ischemia
- quality control
- subarachnoid hemorrhage
- risk factors
- endothelial cells
- cell death
- drug induced
- high frequency
- poor prognosis
- cell therapy
- spinal cord injury
- skeletal muscle
- machine learning
- high fat diet induced
- multiple sclerosis
- stress induced
- drug delivery
- blood brain barrier
- long non coding rna
- mesenchymal stem cells