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2 results on '"adropin"'

1. Adropin: An endocrine link between the biological clock and cholesterol homeostasis

Author

Ghoshal, Sarbani, Stevens, Joseph R, Billon, Cyrielle, Girardet, Clemence, Sitaula, Sadichha, Leon, Arthur S, Rao, DC, Skinner, James S, Rankinen, Tuomo, Bouchard, Claude, Nuñez, Marinelle V, Stanhope, Kimber L, Howatt, Deborah A, Daugherty, Alan, Zhang, Jinsong, Schuelke, Matthew, Weiss, Edward P, Coffey, Alisha R, Bennett, Brian J, Sethupathy, Praveen, Burris, Thomas P, Havel, Peter J, and Butler, Andrew A

Subjects
Biochemistry and Cell Biology, Biological Sciences, Genetics, Atherosclerosis, Nutrition, Digestive Diseases, Liver Disease, Obesity, Prevention, 1.1 Normal biological development and functioning, Metabolic and endocrine, Adult, Aged, Animals, Blood Proteins, Cells, Cultured, Cholesterol, LDL, Circadian Clocks, Female, Glucose, Hep G2 Cells, Homeostasis, Humans, Intercellular Signaling Peptides and Proteins, Liver, Macaca mulatta, Male, Mice, Middle Aged, Nuclear Receptor Subfamily 1, Group F, Member 1, Nuclear Receptor Subfamily 1, Group F, Member 3, Peptides, Proteins, Cholesterol, LDL, Cardiovascular disease, Adropin, Sex, Physiology, Biochemistry and cell biology
Abstract

ObjectiveIdentify determinants of plasma adropin concentrations, a secreted peptide translated from the Energy Homeostasis Associated (ENHO) gene linked to metabolic control and vascular function.MethodsAssociations between plasma adropin concentrations, demographics (sex, age, BMI) and circulating biomarkers of lipid and glucose metabolism were assessed in plasma obtained after an overnight fast in humans. The regulation of adropin expression was then assessed in silico, in cultured human cells, and in animal models.ResultsIn humans, plasma adropin concentrations are inversely related to atherogenic LDL-cholesterol (LDL-C) levels in men (n = 349), but not in women (n = 401). Analysis of hepatic Enho expression in male mice suggests control by the biological clock. Expression is rhythmic, peaking during maximal food consumption in the dark correlating with transcriptional activation by RORα/γ. The nadir in the light phase coincides with the rest phase and repression by Rev-erb. Plasma adropin concentrations in nonhuman primates (rhesus monkeys) also exhibit peaks coinciding with feeding times (07:00 h, 15:00 h). The ROR inverse agonists SR1001 and the 7-oxygenated sterols 7-β-hydroxysterol and 7-ketocholesterol, or the Rev-erb agonist SR9009, suppress ENHO expression in cultured human HepG2 cells. Consumption of high-cholesterol diets suppress expression of the adropin transcript in mouse liver. However, adropin over expression does not prevent hypercholesterolemia resulting from a high cholesterol diet and/or LDL receptor mutations.ConclusionsIn humans, associations between plasma adropin concentrations and LDL-C suggest a link with hepatic lipid metabolism. Mouse studies suggest that the relationship between adropin and cholesterol metabolism is unidirectional, and predominantly involves suppression of adropin expression by cholesterol and 7-oxygenated sterols. Sensing of fatty acids, cholesterol and oxysterols by the RORα/γ ligand-binding domain suggests a plausible functional link between adropin expression and cellular lipid metabolism. Furthermore, the nuclear receptors RORα/γ and Rev-erb may couple adropin synthesis with circadian rhythms in carbohydrate and lipid metabolism.

Published
2018

2. Adropin: An endocrine link between the biological clock and cholesterol homeostasis.

Author

Ghoshal, Sarbani, Stevens, Joseph R, Billon, Cyrielle, Girardet, Clemence, Sitaula, Sadichha, Leon, Arthur S, Rao, DC, Skinner, James S, Rankinen, Tuomo, Bouchard, Claude, Nuñez, Marinelle V, Stanhope, Kimber L, Howatt, Deborah A, Daugherty, Alan, Zhang, Jinsong, Schuelke, Matthew, Weiss, Edward P, Coffey, Alisha R, Bennett, Brian J, Sethupathy, Praveen, Burris, Thomas P, Havel, Peter J, and Butler, Andrew A

Subjects
Liver, Cells, Cultured, Animals, Macaca mulatta, Humans, Mice, Glucose, Intercellular Signaling Peptides and Proteins, Peptides, Proteins, Blood Proteins, Homeostasis, Adult, Aged, Middle Aged, Female, Male, Cholesterol, LDL, Hep G2 Cells, Nuclear Receptor Subfamily 1, Group F, Member 1, Nuclear Receptor Subfamily 1, Group F, Member 3, Circadian Clocks, Adropin, Cardiovascular disease, Cholesterol, LDL, Obesity, Sex, Biochemistry and Cell Biology, Physiology
Abstract

ObjectiveIdentify determinants of plasma adropin concentrations, a secreted peptide translated from the Energy Homeostasis Associated (ENHO) gene linked to metabolic control and vascular function.MethodsAssociations between plasma adropin concentrations, demographics (sex, age, BMI) and circulating biomarkers of lipid and glucose metabolism were assessed in plasma obtained after an overnight fast in humans. The regulation of adropin expression was then assessed in silico, in cultured human cells, and in animal models.ResultsIn humans, plasma adropin concentrations are inversely related to atherogenic LDL-cholesterol (LDL-C) levels in men (n = 349), but not in women (n = 401). Analysis of hepatic Enho expression in male mice suggests control by the biological clock. Expression is rhythmic, peaking during maximal food consumption in the dark correlating with transcriptional activation by RORα/γ. The nadir in the light phase coincides with the rest phase and repression by Rev-erb. Plasma adropin concentrations in nonhuman primates (rhesus monkeys) also exhibit peaks coinciding with feeding times (07:00 h, 15:00 h). The ROR inverse agonists SR1001 and the 7-oxygenated sterols 7-β-hydroxysterol and 7-ketocholesterol, or the Rev-erb agonist SR9009, suppress ENHO expression in cultured human HepG2 cells. Consumption of high-cholesterol diets suppress expression of the adropin transcript in mouse liver. However, adropin over expression does not prevent hypercholesterolemia resulting from a high cholesterol diet and/or LDL receptor mutations.ConclusionsIn humans, associations between plasma adropin concentrations and LDL-C suggest a link with hepatic lipid metabolism. Mouse studies suggest that the relationship between adropin and cholesterol metabolism is unidirectional, and predominantly involves suppression of adropin expression by cholesterol and 7-oxygenated sterols. Sensing of fatty acids, cholesterol and oxysterols by the RORα/γ ligand-binding domain suggests a plausible functional link between adropin expression and cellular lipid metabolism. Furthermore, the nuclear receptors RORα/γ and Rev-erb may couple adropin synthesis with circadian rhythms in carbohydrate and lipid metabolism.

Published
2018

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