Litcius/Paper detail

Hyperexcitable arousal circuits drive sleep instability during aging

Shi‐Bin Li, Valentina Martínez Damonte, Chong Chen, Gordon Wang, Justus M. Kebschull, Hiroshi Yamaguchi, W Bian, Carolin Purmann, Reenal Pattni, Alexander E. Urban, Philippe Mourrain, Julie A. Kauer, Grégory Scherrer, Luı́s de Lecea

2022Science185 citationsDOIOpen Access PDF

Abstract

Sleep quality declines with age; however, the underlying mechanisms remain elusive. We found that hyperexcitable hypocretin/orexin (Hcrt/OX) neurons drive sleep fragmentation during aging. In aged mice, Hcrt neurons exhibited more frequent neuronal activity epochs driving wake bouts, and optogenetic activation of Hcrt neurons elicited more prolonged wakefulness. Aged Hcrt neurons showed hyperexcitability with lower KCNQ2 expression and impaired M-current, mediated by KCNQ2/3 channels. Single-nucleus RNA-sequencing revealed adaptive changes to Hcrt neuron loss in the aging brain. Disruption of Kcnq2/3 genes in Hcrt neurons of young mice destabilized sleep, mimicking aging-associated sleep fragmentation, whereas the KCNQ-selective activator flupirtine hyperpolarized Hcrt neurons and rejuvenated sleep architecture in aged mice. Our findings demonstrate a mechanism underlying sleep instability during aging and a strategy to improve sleep continuity.

Topics & Concepts

OptogeneticsWakefulnessNeuroscienceArousalNeuronOrexinSleep (system call)PsychologyBiologyMedicineInternal medicineElectroencephalographyNeuropeptideComputer scienceOperating systemReceptorSleep and Wakefulness ResearchCircadian rhythm and melatoninNeuroscience of respiration and sleep