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Metabolic response to 36 hours of fasting in young men born small vs appropriate for gestational age
by
Thankamony, Ajay
, Friedrichsen, Martin
, Dunger, David B.
, Bluck, Les
, Færch, Kristine
, Jørgensen, Sine W.
, Gillberg, Linn
, Brøns, Charlotte
, Hjort, Line
, Vaag, Allan A.
in
Adaptation, Physiological
/ Adult
/ Birth weight
/ Birth Weight - physiology
/ Blood Glucose - metabolism
/ Body fat
/ Diabetes
/ DNA methylation
/ Energy
/ Energy Metabolism
/ Epigenetics
/ Fasting
/ Fasting - metabolism
/ Female
/ Gestational age
/ Glucose
/ Human Physiology
/ Humans
/ Hypotheses
/ Infant, Newborn
/ Infant, Small for Gestational Age - metabolism
/ Insulin resistance
/ Insulin Resistance - physiology
/ Internal Medicine
/ Male
/ Medicine
/ Medicine & Public Health
/ Metabolic Diseases
/ Metabolism
/ Nutrition research
/ Pediatrics
/ Pregnancy
/ Time Factors
/ Young Adult
/ Young adults
2015
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Metabolic response to 36 hours of fasting in young men born small vs appropriate for gestational age
by
Thankamony, Ajay
, Friedrichsen, Martin
, Dunger, David B.
, Bluck, Les
, Færch, Kristine
, Jørgensen, Sine W.
, Gillberg, Linn
, Brøns, Charlotte
, Hjort, Line
, Vaag, Allan A.
in
Adaptation, Physiological
/ Adult
/ Birth weight
/ Birth Weight - physiology
/ Blood Glucose - metabolism
/ Body fat
/ Diabetes
/ DNA methylation
/ Energy
/ Energy Metabolism
/ Epigenetics
/ Fasting
/ Fasting - metabolism
/ Female
/ Gestational age
/ Glucose
/ Human Physiology
/ Humans
/ Hypotheses
/ Infant, Newborn
/ Infant, Small for Gestational Age - metabolism
/ Insulin resistance
/ Insulin Resistance - physiology
/ Internal Medicine
/ Male
/ Medicine
/ Medicine & Public Health
/ Metabolic Diseases
/ Metabolism
/ Nutrition research
/ Pediatrics
/ Pregnancy
/ Time Factors
/ Young Adult
/ Young adults
2015
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Metabolic response to 36 hours of fasting in young men born small vs appropriate for gestational age
by
Thankamony, Ajay
, Friedrichsen, Martin
, Dunger, David B.
, Bluck, Les
, Færch, Kristine
, Jørgensen, Sine W.
, Gillberg, Linn
, Brøns, Charlotte
, Hjort, Line
, Vaag, Allan A.
in
Adaptation, Physiological
/ Adult
/ Birth weight
/ Birth Weight - physiology
/ Blood Glucose - metabolism
/ Body fat
/ Diabetes
/ DNA methylation
/ Energy
/ Energy Metabolism
/ Epigenetics
/ Fasting
/ Fasting - metabolism
/ Female
/ Gestational age
/ Glucose
/ Human Physiology
/ Humans
/ Hypotheses
/ Infant, Newborn
/ Infant, Small for Gestational Age - metabolism
/ Insulin resistance
/ Insulin Resistance - physiology
/ Internal Medicine
/ Male
/ Medicine
/ Medicine & Public Health
/ Metabolic Diseases
/ Metabolism
/ Nutrition research
/ Pediatrics
/ Pregnancy
/ Time Factors
/ Young Adult
/ Young adults
2015
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Metabolic response to 36 hours of fasting in young men born small vs appropriate for gestational age
Journal Article
Metabolic response to 36 hours of fasting in young men born small vs appropriate for gestational age
2015
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Overview
Aims/hypothesis
Being born small for gestational age (SGA) is associated with an increased risk of type 2 diabetes in an affluent society, but could confer an improved chance of survival during sparse living conditions. We studied whether insulin action and other metabolic responses to prolonged fasting differed between 21 young adults born SGA and 18 matched controls born appropriate for gestational age (AGA).
Methods
A frequently sampled IVGTT and indirect calorimetry measurements were performed after a 36 h fast. Endogenous glucose production, insulin sensitivity (S
I
), first-phase insulin secretion and glucose effectiveness were estimated by stable isotope tracer techniques and minimal modelling. Muscle and fat biopsies were obtained after 35 h of fasting.
Results
During fasting, SGA individuals experienced a more pronounced decrease in serum insulin and lower plasma triacylglycerol levels compared with AGA individuals. In addition, energy expenditure decreased in SGA but increased in AGA individuals. After fasting, SGA individuals displayed lower fat oxidation than AGA individuals. S
G
was reduced in SGA compared with AGA individuals, whereas hepatic or whole body insulin action (S
I
) did not differ between groups. SGA individuals had increased muscle
PPARGC1A
DNA methylation. We found no differences in adipose tissue
PPARGC1A
DNA methylation, muscle and adipose tissue
PPARGC1A
mRNA expression, or muscle glycogen levels between the groups.
Conclusion
Compared with AGA individuals, SGA individuals displayed a more energy-conserving and energy-conserving cardiometabolic response to 36 h fasting. The role of increased muscle
PPARGC1A
DNA methylation in mediating this response requires further study.
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