19 research outputs found
Neural correlates of arousal-induced circadian clock resetting: hypocretin/orexin and the intergeniculate leaflet
Deletion of presynaptic adenosine A1 receptors impairs the recovery of synaptic transmission after hypoxia
Sleep architecture of the melanin-concentrating hormone receptor 1-knockout mice
Growing amounts of data indicate involvement of the posterior hypothalamus in the regulation of sleep, especially paradoxical sleep
(PS). Accordingly, we previously showed that the melanin-concentrating hormone (MCH)-producing neurons of the rat hypothalamus
are selectively activated during a PS rebound. In addition, intracerebroventricular infusion of MCH increases total sleep duration,
suggesting a new role for MCH in sleep regulation. To determine whether activation of the MCH system promotes sleep, we studied
spontaneous sleep and its homeostatic regulation in mice with deletion of the MCH-receptor 1 gene (MCH-R1– ⁄ – vs. MCH-R1+ ⁄ +)
and their behavioural response to modafinil, a powerful antinarcoleptic drug. Here, we show that the lack of functional MCH-R1
results in a hypersomniac-like phenotype, both in basal conditions and after total sleep deprivation, compared to wild-type mice.
Further, we found that modafinil was less potent at inducing wakefulness in MCH-R1– ⁄ – than in MCH-R1+ ⁄ + mice. We report for the
first time that animals with genetically inactivated MCH signaling exhibit altered vigilance state architecture and sleep homeostasis.
This study also suggests that the MCH system may modulate central pathways involved in the wake-promoting effect of modafini
Sleep modulates haematopoiesis and protects against atherosclerosis.
Sleep is integral to life <sup>1</sup> . Although insufficient or disrupted sleep increases the risk of multiple pathological conditions, including cardiovascular disease <sup>2</sup> , we know little about the cellular and molecular mechanisms by which sleep maintains cardiovascular health. Here we report that sleep regulates haematopoiesis and protects against atherosclerosis in mice. We show that mice subjected to sleep fragmentation produce more Ly-6C <sup>high</sup> monocytes, develop larger atherosclerotic lesions and produce less hypocretin-a stimulatory and wake-promoting neuropeptide-in the lateral hypothalamus. Hypocretin controls myelopoiesis by restricting the production of CSF1 by hypocretin-receptor-expressing pre-neutrophils in the bone marrow. Whereas hypocretin-null and haematopoietic hypocretin-receptor-null mice develop monocytosis and accelerated atherosclerosis, sleep-fragmented mice with either haematopoietic CSF1 deficiency or hypocretin supplementation have reduced numbers of circulating monocytes and smaller atherosclerotic lesions. Together, these results identify a neuro-immune axis that links sleep to haematopoiesis and atherosclerosis