Effects of thiol antioxidant β-mercaptoethanol on diet-induced obese mice
Obesity and insulin resistance are associated with increased oxidant stress. However, treatments of obese subjects with different types of antioxidants often give mixed outcomes. In this work, we sought to determine if long-term supplementation of a thiol antioxidant, β-mercaptoethanol, to diet-indu...
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Published in | Life sciences (1973) Vol. 107; no. 1-2; pp. 32 - 41 |
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Main Authors | , , , , , , |
Format | Journal Article |
Language | English |
Published |
Netherlands
Elsevier Inc
27.06.2014
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Subjects | |
Online Access | Get full text |
ISSN | 0024-3205 1879-0631 1879-0631 |
DOI | 10.1016/j.lfs.2014.04.031 |
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Abstract | Obesity and insulin resistance are associated with increased oxidant stress. However, treatments of obese subjects with different types of antioxidants often give mixed outcomes. In this work, we sought to determine if long-term supplementation of a thiol antioxidant, β-mercaptoethanol, to diet-induced obese mice may improve their health conditions.
Middle-age mice with pre-existing diet-induced obesity were provided with low concentration β-mercaptoethanol (BME) in drinking water for six months. Animals were assessed for body composition, gripping strength, spontaneous physical and metabolic activities, as well as insulin and pyruvate tolerance tests. Markers of inflammation were assessed in plasma, fat tissue, and liver.
BME-treated mice gained less fat mass and more lean mass than the control animals. They also showed increased nocturnal locomotion and respiration, as well as greater gripping strength. BME reduced plasma lipid peroxidation, decreased abdominal fat tissue inflammation, reduced fat infiltration into muscle and liver, and reduced liver and plasma C-reactive protein. However, BME was found to desensitize insulin signaling in vivo, an effect also confirmed by in vitro experiments.
Long-term supplementation of low dose thiol antioxidant BME improved functional outcomes in animals with pre-existing obesity. Additional studies are needed to address the treatment impact on insulin sensitivity if a therapeutic value is to be explored. |
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AbstractList | Obesity and insulin resistance are associated with increased oxidant stress. However, treatments of obese subjects with different types of antioxidants often give mixed outcomes. In this work, we sought to determine if long-term supplementation of a thiol antioxidant, β-mercaptoethanol, to diet-induced obese mice may improve their health conditions.AIMSObesity and insulin resistance are associated with increased oxidant stress. However, treatments of obese subjects with different types of antioxidants often give mixed outcomes. In this work, we sought to determine if long-term supplementation of a thiol antioxidant, β-mercaptoethanol, to diet-induced obese mice may improve their health conditions.Middle-age mice with pre-existing diet-induced obesity were provided with low concentration β-mercaptoethanol (BME) in drinking water for six months. Animals were assessed for body composition, gripping strength, spontaneous physical and metabolic activities, as well as insulin and pyruvate tolerance tests. Markers of inflammation were assessed in plasma, fat tissue, and liver.MAIN METHODSMiddle-age mice with pre-existing diet-induced obesity were provided with low concentration β-mercaptoethanol (BME) in drinking water for six months. Animals were assessed for body composition, gripping strength, spontaneous physical and metabolic activities, as well as insulin and pyruvate tolerance tests. Markers of inflammation were assessed in plasma, fat tissue, and liver.BME-treated mice gained less fat mass and more lean mass than the control animals. They also showed increased nocturnal locomotion and respiration, as well as greater gripping strength. BME reduced plasma lipid peroxidation, decreased abdominal fat tissue inflammation, reduced fat infiltration into muscle and liver, and reduced liver and plasma C-reactive protein. However, BME was found to desensitize insulin signaling in vivo, an effect also confirmed by in vitro experiments.KEY FINDINGSBME-treated mice gained less fat mass and more lean mass than the control animals. They also showed increased nocturnal locomotion and respiration, as well as greater gripping strength. BME reduced plasma lipid peroxidation, decreased abdominal fat tissue inflammation, reduced fat infiltration into muscle and liver, and reduced liver and plasma C-reactive protein. However, BME was found to desensitize insulin signaling in vivo, an effect also confirmed by in vitro experiments.Long-term supplementation of low dose thiol antioxidant BME improved functional outcomes in animals with pre-existing obesity. Additional studies are needed to address the treatment impact on insulin sensitivity if a therapeutic value is to be explored.SIGNIFICANCELong-term supplementation of low dose thiol antioxidant BME improved functional outcomes in animals with pre-existing obesity. Additional studies are needed to address the treatment impact on insulin sensitivity if a therapeutic value is to be explored. Obesity and insulin resistance are associated with increased oxidant stress. However, treatments of obese subjects with different types of antioxidants often give mixed outcomes. In this work, we sought to determine if long-term supplementation of a thiol antioxidant, β-mercaptoethanol, to diet-induced obese mice may improve their health conditions.Middle-age mice with pre-existing diet-induced obesity were provided with low concentration β-mercaptoethanol (BME) in drinking water for six months. Animals were assessed for body composition, gripping strength, spontaneous physical and metabolic activities, as well as insulin and pyruvate tolerance tests. Markers of inflammation were assessed in plasma, fat tissue, and liver.BME-treated mice gained less fat mass and more lean mass than the control animals. They also showed increased nocturnal locomotion and respiration, as well as greater gripping strength. BME reduced plasma lipid peroxidation, decreased abdominal fat tissue inflammation, reduced fat infiltration into muscle and liver, and reduced liver and plasma C-reactive protein. However, BME was found to desensitize insulin signaling in vivo, an effect also confirmed by in vitro experiments.Long-term supplementation of low dose thiol antioxidant BME improved functional outcomes in animals with pre-existing obesity. Additional studies are needed to address the treatment impact on insulin sensitivity if a therapeutic value is to be explored. Obesity and insulin resistance are associated with increased oxidant stress. However, treatments of obese subjects with different types of antioxidants often give mixed outcomes. In this work, we sought to determine if long-term supplementation of a thiol antioxidant, β-mercaptoethanol, to diet-induced obese mice may improve their health conditions. Middle-age mice with pre-existing diet-induced obesity were provided with low concentration β-mercaptoethanol (BME) in drinking water for six months. Animals were assessed for body composition, gripping strength, spontaneous physical and metabolic activities, as well as insulin and pyruvate tolerance tests. Markers of inflammation were assessed in plasma, fat tissue, and liver. BME-treated mice gained less fat mass and more lean mass than the control animals. They also showed increased nocturnal locomotion and respiration, as well as greater gripping strength. BME reduced plasma lipid peroxidation, decreased abdominal fat tissue inflammation, reduced fat infiltration into muscle and liver, and reduced liver and plasma C-reactive protein. However, BME was found to desensitize insulin signaling in vivo, an effect also confirmed by in vitro experiments. Long-term supplementation of low dose thiol antioxidant BME improved functional outcomes in animals with pre-existing obesity. Additional studies are needed to address the treatment impact on insulin sensitivity if a therapeutic value is to be explored. |
Author | Simmons, Amber L. Hamilton, James A. Corkey, Barbara E. Guo, Wen Wong, Siu Schwanz, Heidi A. Kirkland, James L. |
AuthorAffiliation | a Department of Medicine, Boston University School of Medicine, Boston, MA 02118, USA d Research program in Men’s Health, Brigham and Women’s Hospital, Boston, MA 02115, USA b Robert and Arlene Kogod Center on Aging, Mayo Clinic, Rochester, MN 55905, USA c Department of Biophysics, Boston University School of Medicine, Boston, MA 02118, USA |
AuthorAffiliation_xml | – name: b Robert and Arlene Kogod Center on Aging, Mayo Clinic, Rochester, MN 55905, USA – name: a Department of Medicine, Boston University School of Medicine, Boston, MA 02118, USA – name: c Department of Biophysics, Boston University School of Medicine, Boston, MA 02118, USA – name: d Research program in Men’s Health, Brigham and Women’s Hospital, Boston, MA 02115, USA |
Author_xml | – sequence: 1 givenname: Siu surname: Wong fullname: Wong, Siu organization: Department of Medicine, Boston University School of Medicine, Boston, MA 02118, USA – sequence: 2 givenname: James L. surname: Kirkland fullname: Kirkland, James L. organization: Robert and Arlene Kogod Center on Aging, Mayo Clinic, Rochester, MN 55905, USA – sequence: 3 givenname: Heidi A. surname: Schwanz fullname: Schwanz, Heidi A. organization: Department of Biophysics, Boston University School of Medicine, Boston, MA 02118, USA – sequence: 4 givenname: Amber L. surname: Simmons fullname: Simmons, Amber L. organization: Department of Medicine, Boston University School of Medicine, Boston, MA 02118, USA – sequence: 5 givenname: James A. surname: Hamilton fullname: Hamilton, James A. organization: Department of Biophysics, Boston University School of Medicine, Boston, MA 02118, USA – sequence: 6 givenname: Barbara E. surname: Corkey fullname: Corkey, Barbara E. organization: Department of Medicine, Boston University School of Medicine, Boston, MA 02118, USA – sequence: 7 givenname: Wen orcidid: 0000-0002-5998-4257 surname: Guo fullname: Guo, Wen email: wguo2@partners.org organization: Research Program in Men's Health, Brigham and Women's Hospital, Boston, MA 02115, USA |
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Keywords | Gripping strength Diet-induced obesity Thiol antioxidant Insulin resistance Spontaneous locomotion Inflammation β-Mercaptoethanol (PubChem CID: 1567) Respiration Oxidant stress |
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Insulin hypersecretion and food additives: cause of obesity and diabetes? publication-title: Diabetes Care doi: 10.2337/dc12-0825 |
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Snippet | Obesity and insulin resistance are associated with increased oxidant stress. However, treatments of obese subjects with different types of antioxidants often... |
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SubjectTerms | abdominal fat Adipokines - blood Adipose Tissue - drug effects Adipose Tissue - metabolism animal disease models Animals antioxidants Antioxidants - pharmacology beta-mercaptoethanol biochemical pathways blood lipids Body Composition - drug effects C-reactive protein C-Reactive Protein - metabolism Diet, High-Fat Diet-induced obesity Dietary Supplements drinking water Gripping strength Hep G2 Cells Humans Inflammation Inflammation - chemically induced Inflammation - drug therapy insulin Insulin - metabolism Insulin Resistance Lipid Peroxidation liver Liver - drug effects locomotion Locomotion - drug effects Male Mercaptoethanol - pharmacology Mice Mice, Inbred C57BL Mice, Obese Muscle, Skeletal - drug effects muscles obesity Obesity - drug therapy Obesity - metabolism Oxidant stress oxidants pyruvic acid Pyruvic Acid - metabolism Respiration Respiration - drug effects Spontaneous locomotion therapeutics Thiol antioxidant thiols |
Title | Effects of thiol antioxidant β-mercaptoethanol on diet-induced obese mice |
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