Abstract
We have developed a chronic mild stress (MS) mouse model by simply rearing mice on a wire net for 3 weeks and investigated the effects of MS on glucose homeostasis and sleep. MS mice showed impaired glucose tolerance and disturbed sleep. One-week treatment with a histamine H1 receptor antagonist (H1RA) ameliorated the glucose intolerance and improved sleep quality in MS mice. MS mice showed an increased number of mast cells in both adipose tissue and the brain. Inhibition of mast cell function ameliorated the impairment in both glucose tolerance and sleep. Together, these findings indicate that mast cells may represent an important pathophysiological mediator in sleep and energy homeostasis.
Publication types
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Research Support, Non-U.S. Gov't
MeSH terms
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Adipose Tissue / metabolism
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Adipose Tissue / pathology
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Animals
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Brain / drug effects
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Brain / metabolism
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Brain / pathology
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Chronic Disease
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Disease Models, Animal
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Glucose / metabolism*
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Glucose Intolerance / drug therapy
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Glucose Intolerance / metabolism*
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Glucose Intolerance / pathology
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Glucose Tolerance Test
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Histamine H1 Antagonists / pharmacology
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Homeostasis / drug effects
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Homeostasis / physiology
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Male
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Mast Cells / drug effects
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Mast Cells / metabolism*
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Mast Cells / pathology
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Mice, Inbred ICR
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Mice, Transgenic
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Random Allocation
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Sleep Wake Disorders / drug therapy
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Sleep Wake Disorders / metabolism*
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Sleep Wake Disorders / pathology
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Stress, Psychological / drug therapy
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Stress, Psychological / metabolism*
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Stress, Psychological / pathology
Substances
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Histamine H1 Antagonists
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Glucose