Pacific Huynh, Jan D. Hoffmann, Teresa Gerhardt, Máté G. Kiss, Faris M. Zuraikat, Oren Cohen, Christopher Wolfram, Abi G. Yates, Alexander Leunig, Merlin Heiser, Lena Gaebel, Matteo Gianeselli, Sukanya Goswami, Annie Khamhoung, Jeffrey Downey, Seonghun Yoon, Zhihong Chen, Vladimir Roudko, Travis Dawson, Joana Ferreira da Silva, Natalie J. Ameral, Jarod Morgenroth-Rebin, Darwin D’Souza, Laura L. Koekkoek, Walter Jacob, Jazz Munitz, Donghoon Lee, John F. Fullard, Mandy M. T. van Leent, Panos Roussos, Seunghee Kim-Schulze, Neomi Shah, Benjamin P. Kleinstiver, Filip K. Swirski, David Leistner, Marie-Pierre St-Onge, Cameron S. McAlpine
{"title":"心肌梗塞会增加睡眠时间,从而限制心脏炎症和损伤","authors":"Pacific Huynh, Jan D. Hoffmann, Teresa Gerhardt, Máté G. Kiss, Faris M. Zuraikat, Oren Cohen, Christopher Wolfram, Abi G. Yates, Alexander Leunig, Merlin Heiser, Lena Gaebel, Matteo Gianeselli, Sukanya Goswami, Annie Khamhoung, Jeffrey Downey, Seonghun Yoon, Zhihong Chen, Vladimir Roudko, Travis Dawson, Joana Ferreira da Silva, Natalie J. Ameral, Jarod Morgenroth-Rebin, Darwin D’Souza, Laura L. Koekkoek, Walter Jacob, Jazz Munitz, Donghoon Lee, John F. Fullard, Mandy M. T. van Leent, Panos Roussos, Seunghee Kim-Schulze, Neomi Shah, Benjamin P. Kleinstiver, Filip K. Swirski, David Leistner, Marie-Pierre St-Onge, Cameron S. McAlpine","doi":"10.1038/s41586-024-08100-w","DOIUrl":null,"url":null,"abstract":"Sleep is integral to cardiovascular health1,2. Yet, the circuits that connect cardiovascular pathology and sleep are incompletely understood. It remains unclear whether cardiac injury influences sleep and whether sleep-mediated neural outputs contribute to heart healing and inflammation. Here we report that in humans and mice, monocytes are actively recruited to the brain after myocardial infarction (MI) to augment sleep, which suppresses sympathetic outflow to the heart, limiting inflammation and promoting healing. After MI, microglia rapidly recruit circulating monocytes to the brain’s thalamic lateral posterior nucleus (LPN) via the choroid plexus, where they are reprogrammed to generate tumour necrosis factor (TNF). In the thalamic LPN, monocytic TNF engages Tnfrsf1a-expressing glutamatergic neurons to increase slow wave sleep pressure and abundance. Disrupting sleep after MI worsens cardiac function, decreases heart rate variability and causes spontaneous ventricular tachycardia. After MI, disrupting or curtailing sleep by manipulating glutamatergic TNF signalling in the thalamic LPN increases cardiac sympathetic input which signals through the β2-adrenergic receptor of macrophages to promote a chemotactic signature that increases monocyte influx. Poor sleep in the weeks following acute coronary syndrome increases susceptibility to secondary cardiovascular events and reduces the heart’s functional recovery. In parallel, insufficient sleep in humans reprogrammes β2-adrenergic receptor-expressing monocytes towards a chemotactic phenotype, enhancing their migratory capacity. Collectively, our data uncover cardiogenic regulation of sleep after heart injury, which restricts cardiac sympathetic input, limiting inflammation and damage. Studies in humans and mice show that myocardial infarction recruits monocytes to the brain’s thalamus, promoting sleep, which in turn restricts cardiac inflammation and sympathetic signalling and assists healing.","PeriodicalId":18787,"journal":{"name":"Nature","volume":"635 8037","pages":"168-177"},"PeriodicalIF":50.5000,"publicationDate":"2024-10-30","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Myocardial infarction augments sleep to limit cardiac inflammation and damage\",\"authors\":\"Pacific Huynh, Jan D. Hoffmann, Teresa Gerhardt, Máté G. Kiss, Faris M. Zuraikat, Oren Cohen, Christopher Wolfram, Abi G. Yates, Alexander Leunig, Merlin Heiser, Lena Gaebel, Matteo Gianeselli, Sukanya Goswami, Annie Khamhoung, Jeffrey Downey, Seonghun Yoon, Zhihong Chen, Vladimir Roudko, Travis Dawson, Joana Ferreira da Silva, Natalie J. Ameral, Jarod Morgenroth-Rebin, Darwin D’Souza, Laura L. Koekkoek, Walter Jacob, Jazz Munitz, Donghoon Lee, John F. Fullard, Mandy M. T. van Leent, Panos Roussos, Seunghee Kim-Schulze, Neomi Shah, Benjamin P. Kleinstiver, Filip K. Swirski, David Leistner, Marie-Pierre St-Onge, Cameron S. McAlpine\",\"doi\":\"10.1038/s41586-024-08100-w\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"Sleep is integral to cardiovascular health1,2. Yet, the circuits that connect cardiovascular pathology and sleep are incompletely understood. It remains unclear whether cardiac injury influences sleep and whether sleep-mediated neural outputs contribute to heart healing and inflammation. Here we report that in humans and mice, monocytes are actively recruited to the brain after myocardial infarction (MI) to augment sleep, which suppresses sympathetic outflow to the heart, limiting inflammation and promoting healing. After MI, microglia rapidly recruit circulating monocytes to the brain’s thalamic lateral posterior nucleus (LPN) via the choroid plexus, where they are reprogrammed to generate tumour necrosis factor (TNF). In the thalamic LPN, monocytic TNF engages Tnfrsf1a-expressing glutamatergic neurons to increase slow wave sleep pressure and abundance. Disrupting sleep after MI worsens cardiac function, decreases heart rate variability and causes spontaneous ventricular tachycardia. After MI, disrupting or curtailing sleep by manipulating glutamatergic TNF signalling in the thalamic LPN increases cardiac sympathetic input which signals through the β2-adrenergic receptor of macrophages to promote a chemotactic signature that increases monocyte influx. Poor sleep in the weeks following acute coronary syndrome increases susceptibility to secondary cardiovascular events and reduces the heart’s functional recovery. In parallel, insufficient sleep in humans reprogrammes β2-adrenergic receptor-expressing monocytes towards a chemotactic phenotype, enhancing their migratory capacity. Collectively, our data uncover cardiogenic regulation of sleep after heart injury, which restricts cardiac sympathetic input, limiting inflammation and damage. 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Myocardial infarction augments sleep to limit cardiac inflammation and damage
Sleep is integral to cardiovascular health1,2. Yet, the circuits that connect cardiovascular pathology and sleep are incompletely understood. It remains unclear whether cardiac injury influences sleep and whether sleep-mediated neural outputs contribute to heart healing and inflammation. Here we report that in humans and mice, monocytes are actively recruited to the brain after myocardial infarction (MI) to augment sleep, which suppresses sympathetic outflow to the heart, limiting inflammation and promoting healing. After MI, microglia rapidly recruit circulating monocytes to the brain’s thalamic lateral posterior nucleus (LPN) via the choroid plexus, where they are reprogrammed to generate tumour necrosis factor (TNF). In the thalamic LPN, monocytic TNF engages Tnfrsf1a-expressing glutamatergic neurons to increase slow wave sleep pressure and abundance. Disrupting sleep after MI worsens cardiac function, decreases heart rate variability and causes spontaneous ventricular tachycardia. After MI, disrupting or curtailing sleep by manipulating glutamatergic TNF signalling in the thalamic LPN increases cardiac sympathetic input which signals through the β2-adrenergic receptor of macrophages to promote a chemotactic signature that increases monocyte influx. Poor sleep in the weeks following acute coronary syndrome increases susceptibility to secondary cardiovascular events and reduces the heart’s functional recovery. In parallel, insufficient sleep in humans reprogrammes β2-adrenergic receptor-expressing monocytes towards a chemotactic phenotype, enhancing their migratory capacity. Collectively, our data uncover cardiogenic regulation of sleep after heart injury, which restricts cardiac sympathetic input, limiting inflammation and damage. Studies in humans and mice show that myocardial infarction recruits monocytes to the brain’s thalamus, promoting sleep, which in turn restricts cardiac inflammation and sympathetic signalling and assists healing.
期刊介绍:
Nature is a prestigious international journal that publishes peer-reviewed research in various scientific and technological fields. The selection of articles is based on criteria such as originality, importance, interdisciplinary relevance, timeliness, accessibility, elegance, and surprising conclusions. In addition to showcasing significant scientific advances, Nature delivers rapid, authoritative, insightful news, and interpretation of current and upcoming trends impacting science, scientists, and the broader public. The journal serves a dual purpose: firstly, to promptly share noteworthy scientific advances and foster discussions among scientists, and secondly, to ensure the swift dissemination of scientific results globally, emphasizing their significance for knowledge, culture, and daily life.
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