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. 2025 Jul;28(7):1460-1472.
doi: 10.1038/s41593-025-01966-7. Epub 2025 May 27.

Lemborexant ameliorates tau-mediated sleep loss and neurodegeneration in males in a mouse model of tauopathy

Samira Parhizkar  1 Xin Bao  1 Wei Chen  1 Nicholas Rensing  1 Yun Chen  1 Michal Kipnis  1 Sihui Song  1 Grace Gent  1 Eric Tycksen  2 Melissa Manis  1 Choonghee Lee  1 Javier Remolina Serrano  1 Megan E Bosch  1 Emily Franke  1 Carla M Yuede  1   3   4 Eric C Landsness  1 Michael Wong  1 David M Holtzman  5
Affiliations

Lemborexant ameliorates tau-mediated sleep loss and neurodegeneration in males in a mouse model of tauopathy

Samira Parhizkar et al. Nat Neurosci. 2025 Jul.

Abstract

Sleep disturbances are associated with the pathogenesis of neurodegenerative diseases such as Alzheimer's disease and primary tauopathies. Here we demonstrate that administration of the dual orexin receptor antagonist lemborexant in the P301S/E4 mouse model of tauopathy improves tau-associated impairments in sleep-wake behavior. It also protects against chronic reactive microgliosis and brain atrophy in male P301S/E4 mice by preventing abnormal phosphorylation of tau. These neuroprotective effects in males were not observed after administration of the nonorexinergic drug zolpidem that similarly promoted nonrapid eye movement sleep. Furthermore, both genetic ablation of orexin receptor 2 and lemborexant treatment reduced wakefulness and decreased seeding and spreading of phosphorylated tau in the brain of wild-type mice. These findings raise the therapeutic potential of targeting sleep by orexin receptor antagonism to prevent abnormal tau phosphorylation and limit tau-induced damage.

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Conflict of interest statement

Competing interests: D.M.H. is an inventor on a patent licensed by Washington University to C2N Diagnostics on the therapeutic use of anti-tau antibodies; cofounded and is on the scientific advisory board of C2N Diagnostics; is on the scientific advisory board of Denali, Genentech, Cajal Neuroscience and Switch Therapeutics and consults for Pfizer and Roche. The other authors declare no competing interests.

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