研究実績の概要 |
Monoacylglycerol lipase (MAGL) plays an important role in terminating endocannabinoid signaling by catalyzing endocannabinoid 2-acylglycerol to form arachidonic acid, an important mediator of inflammatory responses. To explore whether MAGL inhibition could limit pathological Tau-induced neuroinflammatory changes, rTg4510 mice with overexpressing pathological Tau protein have been treated with JZL-184, an inhibitor of monoacylglycerol lipase (MAGL). PET and MRI were carried out before, during, and after the treatment. The in vivo imaging studies revealed that chronic inhibition of the function of MAGL at an early but not late stage of tauopathy decelerated neurodegeneration. Furthermore, the effect of the treatment on constraining neuroinflammation occurred at five months, early than halting the rate of tau accumulation and rescuing neurons (at 7 months), indicating that MAGL inhibition may exert anti-tau and neuroprotective functions via its anti-inflammatory effects.
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