Postprandial Fatty Acid Metabolism in the Natural History of Type 2 Diabetes (T2D) (AGL11)
January 22, 2025 updated by: André Carpentier, Université de Sherbrooke
Postprandial Fatty Acid Metabolism in the Natural History of Type 2 Diabetes (T2D): Relative Contribution of Dietary vs Systemic Fatty Acids to Lean Tissue Fatty Acid Fluxes and Oxidative vs Non-oxidative Pathways
Lipotoxicity-causing fatty acid overexposure and accretion in lean tissues leads to insulin resistance and impaired pancreatic β-cell function - the hallmarks of T2D - contributing to associated complications such as heart failure, kidney failure and microvascular diseases.
Proper dietary fatty acid (DFA) storage in white adipose tissue (WAT) is now thought to prevent lean-tissue lipotoxicity.
Using novel Positron-Emission Tomography (PET) and stable isotopic tracer methods which were developed in Sherbrooke, the investigator showed that WAT storage of DFA is impaired in people with pre-diabetes or T2D.
The investigator also showed that this impairment is associated with greater cardiac DFA uptake, as well as subclinical left-ventricular systolic and diastolic dysfunction.
Then, It has been found that modest weight loss in pre-diabetics, after a one-year lifestyle intervention, improved WAT DFA storage, curbed cardiac DFA uptake, and restored associated left-ventricular dysfunction.
It has been also found that a 7-day low-saturated fat, low-calorie diet raised insulin sensitivity but did not restore WAT or cardiac DFA metabolism.
Whether WAT DFA storage directly impacts cardiac DFA uptake is not known.
Importantly, the investigator recently uncovered marked sex-specific differences in WAT DFA metabolism.
These may explain, at least in part, sex-related differences in the cardiac DFA uptake, which occurs in pre-diabetes.
Higher spillover of WAT DFA into circulating Non-Esterified Fatty Acid (NEFA) appears to be linked in women to greater cardiac DFA uptake, as opposed to direct cardiac chylomicron triglycerides (TG) uptake in men.
Here, the investigator will isolate and compare organ-specific fatty acid uptake occurring postprandially from chylomicron-TG vs. NEFA pools, as well as the oxidative vs. non-oxidative intracellular metabolic pathways associated with increased cardiac DFA uptake in pre-diabetic men and women.
Study Overview
Status
Status
Completed
Conditions
Conditions
Intervention / Treatment
Intervention / Treatment
Study Type
Study Type
Interventional
Enrollment (Actual)
Enrollment
50
Phase
Phase
- Not Applicable
Contacts and Locations
This section provides the contact details for those conducting the study, and information on where this study is being conducted.
Study Locations
-
-
Quebec
-
Sherbrooke, Quebec, Canada, J1H 5N4
- Centre de Recherche du CHUS
-
-
Participation Criteria
Researchers look for people who fit a certain description, called eligibility criteria. Some examples of these criteria are a person's general health condition or prior treatments.
Eligibility Criteria
Eligibility Criteria
Ages Eligible for Study
45 years to 80 years (Adult, Older Adult)
Accepts Healthy Volunteers
Yes
Description
Inclusion Criteria:
- For healthy subjects: fasting glucose < 5.6, 2-hour post 75g Oral Glucose Tolerance Test (OGTT) glucose < 7.8 mmol/l and HbA1c < 5.8%
- For subject with glucose intolerance (IGT): 2-hour post 75g OGTT glucose at 7.8-11.1 mmol/l on two separate occasions and HbA1c of 6.0 to 6.4%
Exclusion Criteria:
- overt cardiovascular disease as assessed by medical history, physical exam, and abnormal ECG
- treatment with a fibrate, thiazolidinedione, beta-blocker or other drug known to affect lipid or carbohydrate metabolism (except statins, metformin, and other antihypertensive agents that can be safely interrupted)
- presence of liver or renal disease, uncontrolled thyroid disorder, previous pancreatitis, bleeding disorder, or other major illness
- smoking (>1 cigarette/day) and/or consumption of >2 alcoholic beverages per day
- prior history or current fasting plasma cholesterol level > 7 mmol/l or fasting TG > 6 mmol/l
- any other contraindication to temporarily interrupt current meds for lipids or hypertension
- being pregnant
- not be barren
Study Plan
This section provides details of the study plan, including how the study is designed and what the study is measuring.
How is the study designed?
Design Details
- Primary Purpose: Basic Science
- Allocation: Randomized
- Interventional Model: Parallel Assignment
- Masking: None (Open Label)
Number of Arms
4
Arms and Interventions
Participant Group / ArmParticipant Group / Arm |
Intervention / TreatmentIntervention / Treatment |
|---|---|
|
Other: A0: PET/scan with [11C] palmitate
A bolus of 180 MBq of [11C]-acetate at time 90min and PET acquisition
|
A subcutaneous abdominal 0.5-g adipose tissue biopsy will be performed at the end of protocols A0 and A1
At time 0, a standard liquid meal (400 mL, 906 kcal, 33g-fat/34g-protein/101g-carbohydrates i.e. 33%/17%/50% calories) will be drunk over 20 minutes
|
|
Other: A1: PET/scan with [11C] palmitate
A bolus injection of 180 MBq of [11C]-acetate at time 90min, followed by PET acquisition
|
A subcutaneous abdominal 0.5-g adipose tissue biopsy will be performed at the end of protocols A0 and A1
At time 0, a standard liquid meal (400 mL, 906 kcal, 33g-fat/34g-protein/101g-carbohydrates i.e. 33%/17%/50% calories) will be drunk over 20 minutes
oral administration of nicotinic acid (100mg at 0, 30, 60, 90, 120, 180, 240 and 300 min) to minimize WAT intracellular lipolysis
Other Names:
|
|
Other: B0: PET/scan with [18F]-FTHA
At time 0, a standard liquid meal will be drunk over 20 minutes with 70 MBq of 18FTHA .
PET acquisition at time 90 min.
|
At time 0, a standard liquid meal (400 mL, 906 kcal, 33g-fat/34g-protein/101g-carbohydrates i.e. 33%/17%/50% calories) will be drunk over 20 minutes
using i.v.
administration of [7,7,8,8-2H]-palmitate (in 25% human albumin) from time -60 to +360 min
oral administration of [U-13C]-palmitate (0.2 g mixed into the liquid meal) at time 0 min
|
|
Other: B1: PET/scan with [18F]-FTHA
At time 0, a standard liquid meal will be drunk over 20 minutes with 70 MBq of 18FTHA followed by a PET acquisition at time 90 min.
|
At time 0, a standard liquid meal (400 mL, 906 kcal, 33g-fat/34g-protein/101g-carbohydrates i.e. 33%/17%/50% calories) will be drunk over 20 minutes
oral administration of nicotinic acid (100mg at 0, 30, 60, 90, 120, 180, 240 and 300 min) to minimize WAT intracellular lipolysis
Other Names:
using i.v.
administration of [7,7,8,8-2H]-palmitate (in 25% human albumin) from time -60 to +360 min
oral administration of [U-13C]-palmitate (0.2 g mixed into the liquid meal) at time 0 min
|
What is the study measuring?
Primary Outcome Measures
Primary Outcome Measures
Outcome Measure |
Measure Description |
Time Frame |
|---|---|---|
|
Plasma NEFA appearance rate
Time Frame: 2 years
|
NEFA appearance will be measured using i.v.
administration of [7,7,8,8-2H]-palmitate (in 25% human albumin) from time -60 to +360 min, as slightly modified from previous descriptions, using Steele's non steady-state equations.
Blood samples to measure plasma palmitate, oleate, linoleate, and total NEFA levels, [7,7,8,8-2H]-palmitate enrichments by GC/MS-MS.
|
2 years
|
|
Cardiac and hepatic uptake
Time Frame: 2 years
|
will be determined using 11C-palmitate PET/CT.
180 MBq will be administered by bolus injection at postprandial time 90min.
After a transmission scan and regional CT (40mA), a 30-min dynamic list-mode PET acquisition will be performed starting at time 90 min on a 18 cm-high thoraco-abdominal segment to include the left cardiac ventricle and most of the liver on a Philips Gemini TOF PET/CT
|
2 years
|
|
WAT spillover NEFA appearance rates
Time Frame: 2 years
|
WAT spillover NEFA will be determined from oral administration of [U-13C]-palmitate. Blood samples to measure plasma [U-13C]-palmitate and chylomicron-TG [U-13C]-palmitate enrichment by GC/MS-MS |
2 years
|
|
oxidative metabolism of NEFA
Time Frame: 2 years
|
will be assessed by using 13C-palmitate
|
2 years
|
|
cardiac and hepatic DFA uptake
Time Frame: 2 years
|
will be assessed using PET/CT method with oral administration of 18FTHA
|
2 years
|
|
whole-body organ-specific DFA partitioning
Time Frame: 2 years
|
will be determined by whole-body CT (16 mA) followed by PET acquisition of 18FTHA
|
2 years
|
Secondary Outcome Measures
Secondary Outcome Measures
Outcome Measure |
Measure Description |
Time Frame |
|---|---|---|
|
Insulin sensitivity
Time Frame: 2 years
|
will be determined using the HOMA-IR (based on fasting insulin and glucose levels)
|
2 years
|
|
Insulin secretion rate
Time Frame: 2 years
|
will be assessed using deconvolution of plasma C-peptide with standard C-peptide kinetic parameters
|
2 years
|
|
β-cell function
Time Frame: 2 years
|
will be assessed by calculation of the disposition index (DI) that is insulin secretion in response to the ambient insulin
|
2 years
|
|
WAT size
Time Frame: 2 years
|
by biopsy fixed in formalin
|
2 years
|
|
hormonal response
Time Frame: 2 years
|
will be determined using a multiplex assay system
|
2 years
|
|
Lipoprotein lipase activity
Time Frame: 2 years
|
will be assessed as on frozen 150-mg portions from biopsy
|
2 years
|
Collaborators and Investigators
This is where you will find people and organizations involved with this study.
Sponsor
Sponsor
Publications and helpful links
The person responsible for entering information about the study voluntarily provides these publications. These may be about anything related to the study.
General Publications
- Ye RZ, Montastier E, Noll C, Frisch F, Fortin M, Bouffard L, Phoenix S, Guerin B, Turcotte EE, Carpentier AC. Total Postprandial Hepatic Nonesterified and Dietary Fatty Acid Uptake Is Increased and Insufficiently Curbed by Adipose Tissue Fatty Acid Trapping in Prediabetes With Overweight. Diabetes. 2022 Sep 1;71(9):1891-1901. doi: 10.2337/db21-1097.
- Montastier E, Ye RZ, Noll C, Bouffard L, Fortin M, Frisch F, Phoenix S, Guerin B, Turcotte EE, Lewis GF, Carpentier AC. Increased postprandial nonesterified fatty acid efflux from adipose tissue in prediabetes is offset by enhanced dietary fatty acid adipose trapping. Am J Physiol Endocrinol Metab. 2021 Jun 1;320(6):E1093-E1106. doi: 10.1152/ajpendo.00619.2020. Epub 2021 Apr 19.
Helpful Links
- Total Postprandial Hepatic Nonesterified and Dietary Fatty Acid Uptake Is Increased and Insufficiently Curbed by Adipose Tissue Fatty Acid Trapping in Prediabetes With Overweight
- Increased postprandial nonesterified fatty acid efflux from adipose tissue in prediabetes is offset by enhanced dietary fatty acid adipose trapping
Study record dates
These dates track the progress of study record and summary results submissions to ClinicalTrials.gov. Study records and reported results are reviewed by the National Library of Medicine (NLM) to make sure they meet specific quality control standards before being posted on the public website.
Study Major Dates
Study Start (Actual)
Study Start
January 17, 2017
Primary Completion (Actual)
Primary Completion
December 1, 2020
Study Completion (Actual)
Study Completion
May 1, 2021
Study Registration Dates
First Submitted
First Submitted
April 14, 2016
First Submitted That Met QC Criteria
First Submitted That Met QC Criteria
June 16, 2016
First Posted (Estimated)
First Posted
June 21, 2016
Study Record Updates
Last Update Posted (Actual)
Last Update Posted
March 25, 2025
Last Update Submitted That Met QC Criteria
Last Update Submitted That Met QC Criteria
January 22, 2025
Last Verified
Last Verified
January 1, 2025
More Information
Terms related to this study
Additional Relevant MeSH Terms
- Metabolic Diseases
- Glucose Metabolism Disorders
- Hyperglycemia
- Glucose Intolerance
- Physiological Effects of Drugs
- Molecular Mechanisms of Pharmacological Action
- Antimetabolites
- Micronutrients
- Vitamin B Complex
- Vitamins
- Vasodilator Agents
- Hypolipidemic Agents
- Lipid Regulating Agents
- Niacin
- Niacinamide
- Nicotinic Acids
Other Study ID Numbers
Other Study ID Numbers
- 2016-1196
This information was retrieved directly from the website clinicaltrials.gov without any changes. If you have any requests to change, remove or update your study details, please contact register@clinicaltrials.gov. As soon as a change is implemented on clinicaltrials.gov, this will be updated automatically on our website as well.
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