Michael Harrop
Well-known member
https://news.uci.edu/2026/02/05/sleep-disruption-damages-guts-self-repair-ability-via-stress-signals-from-brain/
https://www.cell.com/cell-stem-cell/fulltext/S1934-5909(26)00025-1
https://www.cell.com/cell-stem-cell/fulltext/S1934-5909(26)00025-1
Highlights
• Sleep deprivation triggers intestinal stem cell dysfunction and gut pathologies
• Overactive dorsal motor nucleus of vagus transmits sleep defect signals to the gut
• Excess acetylcholine from vagus nerve triggers 5-hydroxytryptamine spike in the gut
• Elevated 5-hydroxytryptamine induces oxidative stress in intestinal stem cells
Summary
Sleep disturbances are associated with pathogenesis of numerous chronic disorders, including chronic gastrointestinal diseases. However, the mechanism that transmits sleep disturbance-induced aberrant neural signaling from the brain to the gut remains elusive.
We show that acute sleep deprivation (SD) impairs intestinal stem cell (ISC) function, leading to shortening of crypt-villus architecture and Paneth cell loss. We identified the dorsal motor nucleus of vagus (DMV) as the SD-sensitive central nervous system center that transmits sleep effects to the gut. SD aberrantly activates DMV neurons, driving excessive acetylcholine release from the vagus nerve into the gut. Acetylcholine triggers 5-hydroxytryptamine (5-HT) release by enterochromaffin cells and suppresses its reuptake via muscarinic receptors, thereby causing a spike in 5-HT levels. Elevated 5-HT induces excessive oxidative stress in ISCs through its receptor HTR4, promoting gut pathologies.
Overall, we reveal an SD-responsive neural circuit that controls ISCs and identify therapeutic strategies for mitigating SD-related gut diseases.
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