Kisspeptin-10 Protects Brain Barrier After Stroke by Boosting Claudin-10 Protein

Acute ischemic stroke, caused by a blocked blood vessel in the brain, leads to rapid neuronal death and significant neurological deficits. A critical consequence of stroke is the disruption of the blood-brain barrier (BBB), a protective layer of cells that controls what enters the brain. This breakdown allows harmful substances into the brain, exacerbating cerebral edema (brain swelling) and worsening patient outcomes. Current stroke therapies primarily focus on restoring blood flow, but often lack direct strategies to preserve BBB integrity. This study investigates whether Kisspeptin-10 can directly protect the BBB after stroke and identifies its molecular mechanism, specifically focusing on tight junction proteins like Claudin-10.

Treatment with Kisspeptin-10 significantly improved neurological function and substantially reduced the extent of brain damage following stroke. The higher dose of 1.0 mg/kg demonstrated the most potent effects, resulting in a 43% reduction (p<0.001) in infarct volume compared to saline-treated stroke controls. This neuroprotective effect was closely linked to enhanced BBB integrity. Kisspeptin-10 treatment at 1.0 mg/kg significantly preserved the blood-brain barrier, evidenced by a remarkable 65% reduction (p<0.001) in Evans Blue extravasation into the brain parenchyma compared to untreated stroke animals. This crucial protective mechanism was attributed to a significant 2.8-fold increase (p<0.01) in Claudin-10 protein expression and a 1.9-fold increase (p<0.05) in ZO-1 (another tight junction protein) within the ischemic penumbra (the salvageable brain tissue surrounding the infarct core). These findings collectively indicate that Kisspeptin-10 strengthens the tight junctions, which are essential for maintaining the BBB's structural and functional integrity.