Obesity Clinical Trial
Official title:
The Role of Central Reward and Satiety Centers in the Etiology of Obesity: Genetic and Environmental Influences
| Verified date | May 2017 |
| Source | VU University Medical Center |
| Contact | n/a |
| Is FDA regulated | No |
| Health authority | |
| Study type | Observational |
The aim of this study is to investigate the effects of genetic and environmental risk factors on central nervous system (CNS) reward and satiety circuits in the etiology of obesity. The investigators will also investigate to what extent the alterations in CNS reward and satiety circuits are a cause or a consequence of the development of obesity.
| Status | Completed |
| Enrollment | 92 |
| Est. completion date | September 2016 |
| Est. primary completion date | September 2016 |
| Accepts healthy volunteers | Accepts Healthy Volunteers |
| Gender | All |
| Age group | 18 Years to 75 Years |
| Eligibility |
Inclusion Criteria: - Age 18-75 years - Male or female - Stable bodyweight (<5% reported weight change during previous 3 months) - Women: regular menstruation cycle (to exclude possible menstruation cycle effects) - Normal fasting blood glucose Exclusion Criteria: - Left handedness - Known diabetes or abnormal fasting blood glucose - Serious heart, pulmonary, hepatic or renal disease, malignant or hematological disease - Metabolic disorders (uncontrolled adrenal/thyroid disease) - Women: irregular menstruation cycle - Neurological or psychiatric illness - Pregnancy or breast feeding - Alcohol abuse - Nicotine abuse - Claustrophobia or metal implants - Visual disability - Participation in another study - Inability to understand the protocol or to give informed consent - Current/chronic use of following medication: antihyperglycemic agents, glucocorticoids, centrally acting drugs, cytostatics, immune suppressants, potentially addictive medications. |
| Country | Name | City | State |
|---|---|---|---|
| Netherlands | VU University Medical Center | Amsterdam |
| Lead Sponsor | Collaborator |
|---|---|
| VU University Medical Center |
Netherlands,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Other | The difference within obesity-discordant monozygotic (MZ) twin pairs regarding gut microbiota composition | Gut microbiota composition (ratio between various gut microbiota species) will be assessed by identifying microbial phylotypes in a feces sample using 16S ribosomal RNA molecule-based approaches of diagnostic analysis. Function of gut microbiota will be investigated using metaproteomics analysis techniques that include mass-spectroscopy methodologies. Please note: this outcome measure is conditional to available budget. |
Baseline (one measurement) | |
| Other | The difference within obesity-discordant monozygotic (MZ) twin pairs regarding epigenetic changes | Epigenetic changes will be assessed by measuring global DNA methylation (%) and locus specific DNA methylation (%) in regions of selected loci using a mass spectrometry-based method. Loci will be selected on the basis of their previously shown features of epigenetic regulation and their involvement in cardiovascular and metabolic disease. Please note: this outcome measure is conditional to available budget. |
Baseline (one measurement) | |
| Other | The difference between individuals at high versus those at low genetic obesity risk regarding gut microbiota composition | Gut microbiota composition (ratio between various gut microbiota species) will be assessed by identifying microbial phylotypes in a feces sample using 16S ribosomal RNA molecule-based approaches of diagnostic analysis. Function of gut microbiota will be investigated using metaproteomics analysis techniques that include mass-spectroscopy methodologies. Please note: this outcome measure is conditional to available budget. |
Baseline (one measurement) | |
| Other | The difference between individuals at high versus those at low genetic obesity risk regarding epigenetic changes | Epigenetic changes will be assessed by measuring global DNA methylation (%) and locus specific DNA methylation (%) in regions of selected loci using a mass spectrometry-based method. Loci will be selected on the basis of their previously shown features of epigenetic regulation and their involvement in cardiovascular and metabolic disease. Please note: this outcome measure is conditional to available budget. |
Baseline (one measurement) | |
| Primary | The difference in neuronal activity in CNS reward and satiety circuits as represented by BOLD functional magnetic resonance imaging (fMRI) signal change from baseline (%) in response to food-related stimuli within obesity discordant MZ twin pairs. | Baseline (one measurement) | ||
| Primary | The difference in neuronal activity in CNS reward and satiety circuits as represented by BOLD fMRI signal change from baseline (%) in response to food-related stimuli between individuals at high verses low genetic obesity risk. | Baseline (one measurement) | ||
| Primary | The difference in neuronal activity in CNS reward and satiety circuits as represented by BOLD fMRI signal change from baseline (%) in response to food-related stimuli between lean and obese subjects with either high or low genetic obesity risk. | Baseline (one measurement) | ||
| Secondary | The difference within obesity-discordant monozygotic (MZ) twin pairs regarding dietary intake | Dietary intake will be measured as quantitative (kcal/day) and qualitative (energy density (kcal/kg) and macronutrient composition (%)) dietary intake using A) a choice lunch buffet on the visit day and B) the 24 hours recall method on two week days and one weekend day at home. | Baseline (one measurement) | |
| Secondary | The difference within obesity-discordant monozygotic (MZ) twin pairs regarding physical activity level | Physical activity level will be measured as metabolic equivalent of task (METs)-hours per week using seven-day ActiGraph triaxial accelerometry at home. | Baseline (one measurement) | |
| Secondary | The difference within obesity-discordant monozygotic (MZ) twin pairs regarding basal metabolic rate | Basal metabolic rate will be measured in kcal/day using oxygen consumption and carbon dioxide production measured by indirect calorimetry using a ventilated hood system. | Baseline (one measurement) | |
| Secondary | The difference within obesity-discordant monozygotic (MZ) twin pairs regarding fasting circulating biomarker levels | Fasting circulating biomarker levels (glucose (mmol/l), HbA1c (mmol/mol), insulin (pmol/l), C-peptide (nmol/l), glucagon (pmol/l), triglycerides (mmol/l), HDL-cholesterol (mmol/l) and LDL-cholesterol (mmol/l)) will be measured in a fasting blood sample. | Baseline (one measurement) | |
| Secondary | The difference within obesity-discordant monozygotic (MZ) twin pairs regarding autonomic nervous system balance | Autonomic nervous system balance will be assessment based on measurements of A) heart rate variability (HRV; calculated as root mean square of successive R-R interval differences (RMSSD) in ms2); B) respiratory rate (RR; breaths/min) and C) respiratory sinus arrhythmia (RSA; ms) in resting conditions and in response to a mental arithmetic task using an electro- and impedance cardiogram. | Baseline (one measurement) | |
| Secondary | The difference between individuals at high versus those at low genetic obesity risk regarding dietary intake | Dietary intake will be measured as quantitative (kcal/day) and qualitative (energy density (kcal/kg) and macronutrient composition (%)) dietary intake using A) a choice lunch buffet on the visit day and B) the 24 hours recall method on two week days and one weekend day at home. | Baseline (one measurement) | |
| Secondary | The difference between individuals at high versus those at low genetic obesity risk regarding physical activity level | Physical activity level will be measured as metabolic equivalent of task (METs)-hours per week using seven-day ActiGraph triaxial accelerometry at home. | Baseline (one measurement) | |
| Secondary | The difference between individuals at high versus those at low genetic obesity risk regarding basal metabolic rate | Basal metabolic rate will be measured in kcal/day using oxygen consumption and carbon dioxide production measured by indirect calorimetry using a ventilated hood system. | Baseline (one measurement) | |
| Secondary | The difference between individuals at high versus those at low genetic obesity risk regarding fasting circulating biomarker levels | Fasting circulating biomarker levels (glucose (mmol/l), HbA1c (mmol/mol), insulin (pmol/l), C-peptide (nmol/l), glucagon (pmol/l), triglycerides (mmol/l), HDL-cholesterol (mmol/l) and LDL-cholesterol (mmol/l)) will be measured in a fasting blood sample. | Baseline (one measurement) | |
| Secondary | The difference between individuals at high versus those at low genetic obesity risk regarding autonomic nervous system balance | Autonomic nervous system balance will be assessment based on measurements of A) heart rate variability (HRV; calculated as root mean square of successive R-R interval differences (RMSSD) in ms2); B) respiratory rate (RR; breaths/min) and C) respiratory sinus arrhythmia (RSA; ms) in resting conditions and in response to a mental arithmetic task using an electro- and impedance cardiogram. | Baseline (one measurement) |
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