Sleep restriction does not affect orthostatic tolerance in the simulated microgravity environment

1 Division of Endocrinology, Hypertension and Diabetes, Brigham and Women's Hospital, Boston 02115; and 2 NASA Center for Quantitative Cardiovascular Physiology, Modeling and Data Analysis, Harvard-MIT Division of Health Sciences and Technology, Massachusetts Institute of Technology, Cambridge,...

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Published in	Journal of applied physiology (1985) Vol. 97; no. 5; pp. 1660 - 1666
Main Authors	Grenon, S. Marlene, Hurwitz, Shelley, Sheynberg, Natalie, Xiao, Xinshu, Judson, Brad, Ramsdell, Craig D, Kim, Christine, Cohen, Richard J, Williams, Gordon H
Format	Journal Article
Language	English
Published	Bethesda, MD Am Physiological Soc 01.11.2004 American Physiological Society
Subjects	Adult Applied physiology Bed Rest Biological and medical sciences Cardiovascular system Cardiovascular System - physiopathology Endocrine Glands - physiopathology Excretion Gravity Head-Down Tilt Human physiology applied to population studies and life conditions. Human ecophysiology Humans Hypotension, Orthostatic - physiopathology Hypotension, Orthostatic - urine Kidney - physiopathology Male Medical sciences Potassium - urine Renin - urine Simulation Sleep Sleep Deprivation Sleep disorders Sodium - urine Transports. Aerospace. Diving. Altitude Weightlessness Simulation Human Crew Deprivation Astronaut Mineralocorticoid Environmental factor Weightlessness Space flight Aldosterone renin-angiotensin-aldosterone system Renin angiotensin system Sleep Simulation autonomic function Orthostatic tolerance Microgravity NASA Discipline Cardiopulmonary Non-NASA Center
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ISSN	8750-7587 1522-1601
DOI	10.1152/japplphysiol.00328.2004

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Abstract	1 Division of Endocrinology, Hypertension and Diabetes, Brigham and Women's Hospital, Boston 02115; and 2 NASA Center for Quantitative Cardiovascular Physiology, Modeling and Data Analysis, Harvard-MIT Division of Health Sciences and Technology, Massachusetts Institute of Technology, Cambridge, Massachusetts 02139; and 3 Department of Cardio-Thoracic Surgery, McGill University, Montreal, Quebec, Canada H3G 1A4 Submitted 25 March 2004 ; accepted in final form 23 June 2004 Orthostatic intolerance (OI) is a major problem following spaceflight, and, during flight, astronauts also experience sleep restriction. We hypothesized that sleep restriction will compound the risk and severity of OI following simulated microgravity and exaggerate the renal, cardioendocrine, and cardiovascular adaptive responses to it. Nineteen healthy men were equilibrated on a constant diet, after which they underwent a tilt-stand test. They then completed 1416 days of simulated microgravity [head-down tilt bed rest (HDTB)], followed by repeat tilt-stand test. During HDTB, 11 subjects were assigned to an 8-h sleep protocol (non-sleep restricted), and 8 were assigned to a sleep-restricted protocol with 6 h of sleep per night. During various phases, the following were performed: 24-h urine collections, hormonal measurements, and cardiovascular system identification. Development of presyncope or syncope defined OI. There was a significant decrease in time free of OI ( P = 0.02) and an increase in OI occurrence ( P = 0.06) after HDTB among all subjects. However, the increase in OI occurrence did not differ significantly between the two groups ( P = 0.60). The two groups also experienced similar physiological changes with HDTB (initial increase in sodium excretion; increased excretion of potassium at the end of HDTB; increase in plasma renin activity secretion without a change in serum or urine aldosterone). No significant change in autonomic function or catecholamines was noted. Simulated microgravity leads to increased OI, and sleep restriction does not additively worsen OI in simulated microgravity. Furthermore, conditions of sleep restriction and nonsleep restriction are similar with respect to renal, cardioendocrine, and cardiovascular responses to simulated microgravity. renin-angiotensin-aldosterone system; autonomic function Address for reprint requests and other correspondence: G. H. Williams, Division of Endocrinology, Hypertension and Diabetes, BWH, 221 Longwood Ave., Boston, MA 02115 (E-mail: gwilliams{at}partners.org ).
AbstractList	Orthostatic intolerance (OI) is a major problem following spaceflight, and, during flight, astronauts also experience sleep restriction. We hypothesized that sleep restriction will compound the risk and severity of OI following simulated microgravity and exaggerate the renal, cardioendocrine, and cardiovascular adaptive responses to it. Nineteen healthy men were equilibrated on a constant diet, after which they underwent a tilt-stand test. They then completed 14–16 days of simulated microgravity [head-down tilt bed rest (HDTB)], followed by repeat tilt-stand test. During HDTB, 11 subjects were assigned to an 8-h sleep protocol (non-sleep restricted), and 8 were assigned to a sleep-restricted protocol with 6 h of sleep per night. During various phases, the following were performed: 24-h urine collections, hormonal measurements, and cardiovascular system identification. Development of presyncope or syncope defined OI. There was a significant decrease in time free of OI ( P = 0.02) and an increase in OI occurrence ( P = 0.06) after HDTB among all subjects. However, the increase in OI occurrence did not differ significantly between the two groups ( P = 0.60). The two groups also experienced similar physiological changes with HDTB (initial increase in sodium excretion; increased excretion of potassium at the end of HDTB; increase in plasma renin activity secretion without a change in serum or urine aldosterone). No significant change in autonomic function or catecholamines was noted. Simulated microgravity leads to increased OI, and sleep restriction does not additively worsen OI in simulated microgravity. Furthermore, conditions of sleep restriction and nonsleep restriction are similar with respect to renal, cardioendocrine, and cardiovascular responses to simulated microgravity. Orthostatic intolerance (OI) is a major problem following spaceflight, and, during flight, astronauts also experience sleep restriction. We hypothesized that sleep restriction will compound the risk and severity of OI following simulated microgravity and exaggerate the renal, cardioendocrine, and cardiovascular adaptive responses to it. Nineteen healthy men were equilibrated on a constant diet, after which they underwent a tilt-stand test. They then completed 14-16 days of simulated microgravity [head-down tilt bed rest (HDTB)], followed by repeat tilt-stand test. During HDTB, 11 subjects were assigned to an 8-h sleep protocol (non-sleep restricted), and 8 were assigned to a sleep-restricted protocol with 6 h of sleep per night. During various phases, the following were performed: 24-h urine collections, hormonal measurements, and cardiovascular system identification. Development of presyncope or syncope defined OI. There was a significant decrease in time free of OI (P = 0.02) and an increase in OI occurrence (P = 0.06) after HDTB among all subjects. However, the increase in OI occurrence did not differ significantly between the two groups (P = 0.60). The two groups also experienced similar physiological changes with HDTB (initial increase in sodium excretion; increased excretion of potassium at the end of HDTB; increase in plasma renin activity secretion without a change in serum or urine aldosterone). No significant change in autonomic function or catecholamines was noted. Simulated microgravity leads to increased OI, and sleep restriction does not additively worsen OI in simulated microgravity. Furthermore, conditions of sleep restriction and nonsleep restriction are similar with respect to renal, cardioendocrine, and cardiovascular responses to simulated microgravity.Orthostatic intolerance (OI) is a major problem following spaceflight, and, during flight, astronauts also experience sleep restriction. We hypothesized that sleep restriction will compound the risk and severity of OI following simulated microgravity and exaggerate the renal, cardioendocrine, and cardiovascular adaptive responses to it. Nineteen healthy men were equilibrated on a constant diet, after which they underwent a tilt-stand test. They then completed 14-16 days of simulated microgravity [head-down tilt bed rest (HDTB)], followed by repeat tilt-stand test. During HDTB, 11 subjects were assigned to an 8-h sleep protocol (non-sleep restricted), and 8 were assigned to a sleep-restricted protocol with 6 h of sleep per night. During various phases, the following were performed: 24-h urine collections, hormonal measurements, and cardiovascular system identification. Development of presyncope or syncope defined OI. There was a significant decrease in time free of OI (P = 0.02) and an increase in OI occurrence (P = 0.06) after HDTB among all subjects. However, the increase in OI occurrence did not differ significantly between the two groups (P = 0.60). The two groups also experienced similar physiological changes with HDTB (initial increase in sodium excretion; increased excretion of potassium at the end of HDTB; increase in plasma renin activity secretion without a change in serum or urine aldosterone). No significant change in autonomic function or catecholamines was noted. Simulated microgravity leads to increased OI, and sleep restriction does not additively worsen OI in simulated microgravity. Furthermore, conditions of sleep restriction and nonsleep restriction are similar with respect to renal, cardioendocrine, and cardiovascular responses to simulated microgravity. Orthostatic intolerance (OI) is a major problem following spaceflight, and, during flight, astronauts also experience sleep restriction. We hypothesized that sleep restriction will compound the risk and severity of OI following simulated microgravity and exaggerate the renal, cardioendocrine, and cardiovascular adaptive responses to it. Nineteen healthy men were equilibrated on a constant diet, after which they underwent a tilt-stand test. They then completed 14-16 days of simulated microgravity [head-down tilt bed rest (HDTB)], followed by repeat tilt-stand test. During HDTB, 11 subjects were assigned to an 8-h sleep protocol (non-sleep restricted), and 8 were assigned to a sleep-restricted protocol with 6 h of sleep per night. During various phases, the following were performed: 24-h urine collections, hormonal measurements, and cardiovascular system identification. Development of presyncope or syncope defined OI. There was a significant decrease in time free of OI (P = 0.02) and an increase in OI occurrence (P = 0.06) after HDTB among all subjects. However, the increase in OI occurrence did not differ significantly between the two groups (P = 0.60). The two groups also experienced similar physiological changes with HDTB (initial increase in sodium excretion; increased excretion of potassium at the end of HDTB; increase in plasma renin activity secretion without a change in serum or urine aldosterone). No significant change in autonomic function or catecholamines was noted. Simulated microgravity leads to increased OI, and sleep restriction does not additively worsen OI in simulated microgravity. Furthermore, conditions of sleep restriction and nonsleep restriction are similar with respect to renal, cardioendocrine, and cardiovascular responses to simulated microgravity. [PUBLICATION ABSTRACT] 1 Division of Endocrinology, Hypertension and Diabetes, Brigham and Women's Hospital, Boston 02115; and 2 NASA Center for Quantitative Cardiovascular Physiology, Modeling and Data Analysis, Harvard-MIT Division of Health Sciences and Technology, Massachusetts Institute of Technology, Cambridge, Massachusetts 02139; and 3 Department of Cardio-Thoracic Surgery, McGill University, Montreal, Quebec, Canada H3G 1A4 Submitted 25 March 2004 ; accepted in final form 23 June 2004 Orthostatic intolerance (OI) is a major problem following spaceflight, and, during flight, astronauts also experience sleep restriction. We hypothesized that sleep restriction will compound the risk and severity of OI following simulated microgravity and exaggerate the renal, cardioendocrine, and cardiovascular adaptive responses to it. Nineteen healthy men were equilibrated on a constant diet, after which they underwent a tilt-stand test. They then completed 1416 days of simulated microgravity [head-down tilt bed rest (HDTB)], followed by repeat tilt-stand test. During HDTB, 11 subjects were assigned to an 8-h sleep protocol (non-sleep restricted), and 8 were assigned to a sleep-restricted protocol with 6 h of sleep per night. During various phases, the following were performed: 24-h urine collections, hormonal measurements, and cardiovascular system identification. Development of presyncope or syncope defined OI. There was a significant decrease in time free of OI ( P = 0.02) and an increase in OI occurrence ( P = 0.06) after HDTB among all subjects. However, the increase in OI occurrence did not differ significantly between the two groups ( P = 0.60). The two groups also experienced similar physiological changes with HDTB (initial increase in sodium excretion; increased excretion of potassium at the end of HDTB; increase in plasma renin activity secretion without a change in serum or urine aldosterone). No significant change in autonomic function or catecholamines was noted. Simulated microgravity leads to increased OI, and sleep restriction does not additively worsen OI in simulated microgravity. Furthermore, conditions of sleep restriction and nonsleep restriction are similar with respect to renal, cardioendocrine, and cardiovascular responses to simulated microgravity. renin-angiotensin-aldosterone system; autonomic function Address for reprint requests and other correspondence: G. H. Williams, Division of Endocrinology, Hypertension and Diabetes, BWH, 221 Longwood Ave., Boston, MA 02115 (E-mail: gwilliams{at}partners.org ).
Author	Sheynberg, Natalie Grenon, S. Marlene Judson, Brad Ramsdell, Craig D Xiao, Xinshu Kim, Christine Cohen, Richard J Hurwitz, Shelley Williams, Gordon H
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Keywords	Human Crew Deprivation Astronaut Mineralocorticoid Environmental factor Weightlessness Space flight Aldosterone renin-angiotensin-aldosterone system Renin angiotensin system Sleep Simulation autonomic function Orthostatic tolerance Microgravity NASA Discipline Cardiopulmonary Non-NASA Center
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Snippet	1 Division of Endocrinology, Hypertension and Diabetes, Brigham and Women's Hospital, Boston 02115; and 2 NASA Center for Quantitative Cardiovascular... Orthostatic intolerance (OI) is a major problem following spaceflight, and, during flight, astronauts also experience sleep restriction. We hypothesized that...
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SubjectTerms	Adult Applied physiology Bed Rest Biological and medical sciences Cardiovascular system Cardiovascular System - physiopathology Endocrine Glands - physiopathology Excretion Gravity Head-Down Tilt Human physiology applied to population studies and life conditions. Human ecophysiology Humans Hypotension, Orthostatic - physiopathology Hypotension, Orthostatic - urine Kidney - physiopathology Male Medical sciences Potassium - urine Renin - urine Simulation Sleep Sleep Deprivation Sleep disorders Sodium - urine Transports. Aerospace. Diving. Altitude Weightlessness Simulation
Title	Sleep restriction does not affect orthostatic tolerance in the simulated microgravity environment
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