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El ensayo clínico NCT05041491 (BURST2D) para Pre-diabetes está reclutando. Consulte la vista de tarjeta del Radar de Ensayos Clínicos y las herramientas de descubrimiento de IA para conocer todos los detalles. O haga cualquier pregunta aquí. | ||
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Universidad de Colorado en DenverBreaking up Sedentary Time to Improve Glucose Control in a Population at Risk for Developing Type 2 Diabetes (BURST2D)
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El ensayo clínico NCT05041491 (BURST2D) está diseñado para estudiar la prevención de Pre-diabetes. Es un estudio intervencionista de Fase I temprana. Su estado actual es: reclutando. El ensayo se inició el 30 de noviembre de 2021, con el objetivo de reclutar a 66 participantes. Dirigido por la Universidad de Colorado en Denver, se espera que finalice el 30 de noviembre de 2026. Los datos se actualizaron por última vez en ClinicalTrials.gov el 29 de julio de 2025.
Resumen
Newly released guidelines recommend increased physical activity (PA) and reduced sedentary behaviors (SB) to improve glycemia and prevent the onset and progression of type 2 diabetes (T2D). Typically, 30-60 min bouts of PA are advocated per day. Although this approach increases PA, it does not decrease the length of the sedentary periods through the day. This is important because recent epidemiological data suggest that frequently interrupting sedentary time improves glucose control even in people who achieve the recommended levels of PA. Preliminary experimental data suggest that breaking up prolonged sedentary time by performing multiple short bouts (5 min) of PA throughout the day, may improve glycemia more than performing a single continuous bout of PA, and thereby potentially be a novel strategy to prevent T2D. The improvement in glycemia was observed even when the total amount of PA and total energy expenditure were matched, suggesting that how and when PA is performed over the day may matter more than how much PA is done. However, important gaps in knowledge remain including: (1) whether similar benefits on glucose control would be observed in adults with prediabetes, a clinically relevant population that is at high risk of developing T2D; (2) whether these effects are sustained or diluted over time, and (3) what are the mechanistic underpinnings. To address these gaps, the investigators propose to measure the acute and chronic effects of PA breaks on glucose control and the underlying mechanisms in individuals at risk of developing T2D. Sedentary men and women with prediabetes (n=66, 50% F) will be randomized to either an intervention designed to interrupt SB with 5-min bouts of brisk walking performed hourly for 9 hours/day, 5 days/week (BREAK) or a control condition consisting of 45-min of brisk walking performed as a single daily continuous bout, 5 days/week (ONE). The two 3-months interventions will be matched for total active time.
Título oficial
Breaking up Sedentary Time to Improve Glucose Control in a Population at Risk for Developing Type 2 Diabetes
Condiciones médicas
Pre-diabetesOtros ID del ensayo
- BURST2D
- 20-1900
Número del NCT
Inicio del ensayo (real)
2021-11-30
Última actualización
2025-07-29
Fecha de finalización (estimada)
2026-11-30
Inscripción (prevista)
66
Tipo de estudio
Intervencionista
FASE
Fase I temprana
Estado general
Reclutando
Palabras clave
sedentary behavior
physical activity
glucose control
metabolism
pre-diabetes
physical activity
glucose control
metabolism
pre-diabetes
Objetivo principal
Prevención
Método de asignación
Aleatorizado
Modelo de intervención
Paralelo
Enmascaramiento
Simple
Brazos / Intervenciones
| Grupo de participantes | Intervención/Tratamiento |
|---|---|
ExperimentalBREAK Intervention Participants in the BREAK condition will perform 5-minute bouts of brisk walking hourly for 9 hours/day, 5 days/week for 3 months. | BREAK The BREAK intervention is a physical activity regimen. |
Comparador activoONE Intervention Participants in the ONE condition will perform 45 minutes of brisk walking as a single continuous bout, 5 days/week for 3 months. | ONE The ONE intervention is a physical activity regimen. |
Resultado primario
Resultado secundario
| Medida de resultado | Descripción de la medida | Periodo de tiempo |
|---|---|---|
Glycemia | Plasma glucose concentration in mg/dL measured before and 30, 60, 90 and 120 min after an oral glucose tolerance test (OGTT, 75g glucose). | Glucose concentration in mg/dl, measured at fasting, during a 2 hour OGTT and after |
| Medida de resultado | Descripción de la medida | Periodo de tiempo |
|---|---|---|
Insulinemia | Plasma insulin concentration in milli-international units per milliliter (mUI/mL) measured before and 30, 60, 90 and 120 min after an oral glucose tolerance test (OGTT, 75g glucose). | Plasma insulin concentration in mUI/mL, measured at fasting, during a 2 hour OGTT and after |
Mean interstitial glucose concentration | Mean interstitial glucose concentration measured continuously by a glucose monitor placed on the tricep for 24hours for 10 days. | Before and after 1 month and 3 months of intervention |
Daily glycemia variability | Standard deviation (SD) of interstitial glucose concentration measured continuously by a glucose monitor placed on the tricep 24hours throughout 10 days. | Before and after 1 month and 3 months of intervention |
Fasting A1c concentration | Fasting A1c concentration expressed in % | Time Frame: Before and after 1 month and 3 months of intervention |
Fasting fructosamine concentration | Fasting fructosamine concentration in umol/L | Before and after 1 month and 3 months of intervention |
12-hour exogenous glucose oxidation | Rates of carbon-13 (13C) recovery (% of the dose) in expired carbon dioxide (CO2) following the ingestion of U-13C-glucose in both breakfast and lunch meals. | Before and after 1 month of intervention |
12-hour endogenous glucose oxidation | Rates of D2 recovery (% of the dose) in expired urines following the infusion of (2,2H2) glucose. | Before and after 1 month of intervention |
12 hour CO2 production | CO2 production measured by indirect calorimetry (ParvoMedics TrueOne® 2400, Salt Lake City) for 20 minutes every hour from 0800h to 1800h. | Before and after 1 month of intervention |
12 hour O2 production | O2 production measured by indirect calorimetry (ParvoMedics TrueOne 2400, Salt Lake City) for 20 minutes every hour from 0800h to 1800h. | Before and after 1 month of intervention |
12 Urine excretion | Urine will be measured every hour from 0730h to 1830h | Before and after 1 month of intervention |
Glucose kinetics | Steele's equation for non-steady-state will be used to compute rate of appearance of total glucose (RaT) and rate of appearance of exogenous glucose (RaE), as well as the rates of disappearance (RdT and RdE) from the percentage of \[6,6-2H2\]glucose6 and of 13C-glucose in plasma glucose61. Endogenous glucose production (EGP) will be computed as RaT-RaE. Nonoxidative glucose disposal (NOGD) will be calculated by subtracting total carbohydrate oxidation from (RdT + RdE). Plasma glucose utilization will be assumed to be equivalent to RdT as has been confirmed previously. Muscle glycogen utilization during the active period will be calculated as total carbohydrate utilization during exercise minus plasma glucose utilization during exercise. | Before and after 1 month of intervention |
Fasting and postprandial glucose | Fasting and postprandial glucose in mg/dl measured in response to standard lunch | Before and after 1 month of intervention |
Fasting and postprandial insulin | Fasting and postprandial insulin in ml/iu measured in response to standard lunch | Before and after 1 month of intervention |
Fasting and postprandial C-Peptide | Fasting and postprandial C-peptide nmol/mL measured in response to standard lunch | Before and after 1 month of intervention |
Fasting and postprandial glucagon | Fasting and postprandial glucagon in pg/mL measured in response to standard lunch | Before and after 1 month of intervention |
Fasting and postprandial catecholamines | Fasting and postprandial catecholamines in pg/mL measured in response to standard lunch | Before and after 1 month of intervention |
Skeletal muscle content of protein kinase B (Akt) (Aktser473/total) | Vastus lateralis skeletal muscle biopsies will be collected from fasting participants by the Bergstrom technique. Biopsies will be used to measure protein kinase B (Akt) (Aktser473/total) using western blotting. | Before and after 1 month of intervention |
Skeletal muscle content of ACC (ACCS79/ total) | Vastus lateralis skeletal muscle biopsies will be collected from fasting participants by the Bergstrom technique. Biopsies will be used to measure ACC (ACCS79/ total) using western blotting. | Before and after 1 month of intervention |
Skeletal muscle content of TBC1D4 (AS160/ total) | Vastus lateralis skeletal muscle biopsies will be collected from fasting participants by the Bergstrom technique. Biopsies will be used to measure TBC1D4 (AS160/ total) using western blotting. | Before and after 1 month of intervention |
Skeletal muscle content of COX4 | Vastus lateralis skeletal muscle biopsies will be collected from fasting participants by the Bergstrom technique. Biopsies will be used to measure citrate synthase (COX4) using western blotting. | Before and after 1 month of intervention |
Criterios de elegibilidad
Criterios de edad
Adulto
Edad mínima
18 Years
Criterios de sexo
Todos
- Male and female
- BMI of 18.5-40 kg/m2 and weight stable over the previous 6 months.
- Age, 18-64 years old.
- Fasting glucose of 100-125 mg/dL or fasting HbA1c of 5.7-6.4%, or 2h OGTT blood glucose of 140-199mg/dL based on the American Diabetes Association criteria for pre-diabetes. Fasting glucose, HbA1c and OGTT results ordered by the participant's provider within 3-months of the screening visit will be accepted, provided they fall within the measurement of error range established by the institution's lab standards. Additionally, consistent use of Metformin (1 year) to prevent prediabetes from developing diabetes will be accepted.
- Less than 150 minutes of moderate-to-vigorous physical activity (MVPA) per week and more than 6 hours of sitting time per day, as self-reported by the volunteers using the International Physical Activity Questionnaire (IPAQ).
- Less than 6500 of steps per day as measured by a pedometer over 5 days (at least 1 weekend day).
- Passing medical and physical screening, and analysis of blood and urine screening samples.
- Low-moderate caffeine use (<3 cups/day).
- Agree to refrain from any other structured exercise than the physical activity prescribed in each arm of the study.
- Agree to eat control diets for 3 days before and during the Clinical and Translational Research Center (CTRC) visits;
- Agree to refrain from taking any over-the-counter (including nonsteroidal anti-inflammatory drugs) or prescribed medication (apart from oral contraceptives) for 3 days prior to the inpatient CTRC visits;
- Agree to wear a Fitbit® activity monitor and upload data on the website on a daily basis for the whole duration of the study.
- Agree to follow the physical activity interventions and to be randomly assigned to one of the two arms of the study.
- Agree to complete all the study procedures.
- Pregnancy, breast-feeding or post-menopause for women.
- Being considered unsafe to participate as determined by the study physician.
- Ever having a history of systemic, psychiatric, neurological disease, or drug and alcohol abuse.
- History of cardiovascular disease, diabetes, uncontrolled hypertension, untreated thyroid, renal, hepatic diseases, dyslipidemia or any other medical condition affecting weight or lipid metabolism.
- Being positive for human immunodeficiency virus or hepatitis B or C.
- Taking medications affecting weight, triglycerides, energy intake/energy expenditure, or sleep in the last 3 months.
- Having abnormal blood chemistry and/or hematology as deemed significant by the study physician.
- Being a smoker or having been a smoker in the 3 months prior to their screening visit.
- Having donated over 400 mL of blood within 3 months (90 days) of screening for the study;
- Working night shifts within 1 month of and throughout the study.
- Not completing the trial days of BREAK and ONE during the screening period to assess the willingness and ability of the participant to perform each of the interventions.
Universidad de Colorado en Denver489 ensayos clínicos activos para explorarContactos centrales del ensayo
Contacto: Patricia Smith, MS, RDN, 303.724.6821, [email protected]
Contacto: Audrey Bergouignan, PhD, 303.724.9026, [email protected]
1 Sitios del ensayo en 1 países
Colorado
University of Colorado Anschutz Medical Campus, Aurora, Colorado, 80045, United States
Audrey Bergouignan, PhD, Investigador principal
Reclutando