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 inLife sciences (1973) Vol. 107; no. 1-2; pp. 32 - 41
Main Authors Wong, Siu, Kirkland, James L., Schwanz, Heidi A., Simmons, Amber L., Hamilton, James A., Corkey, Barbara E., Guo, Wen
Format Journal Article
LanguageEnglish
Published Netherlands Elsevier Inc 27.06.2014
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Online AccessGet full text
ISSN0024-3205
1879-0631
1879-0631
DOI10.1016/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.
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
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Issue 1-2
Keywords Gripping strength
Diet-induced obesity
Thiol antioxidant
Insulin resistance
Spontaneous locomotion
Inflammation
β-Mercaptoethanol (PubChem CID: 1567)
Respiration
Oxidant stress
Language English
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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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StartPage 32
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
URI https://dx.doi.org/10.1016/j.lfs.2014.04.031
https://www.ncbi.nlm.nih.gov/pubmed/24802126
https://www.proquest.com/docview/1536682447
https://www.proquest.com/docview/2101398198
https://pubmed.ncbi.nlm.nih.gov/PMC4327985
Volume 107
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