Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT04657939 |
| Other study ID # |
265208 |
| Secondary ID |
18/000590819/WM/ |
| Status |
Completed |
| Phase |
Phase 4
|
| First received |
|
| Last updated |
|
| Start date |
December 1, 2020 |
| Est. completion date |
October 31, 2022 |
Study information
| Verified date |
February 2023 |
| Source |
University of Leeds |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
The majority of people with type 2 diabetes (T2D) are overweight, and while weight gain is a
major contributor to diabetes, a minority of patients with T2D are not overweight or obese.
The reasons why lean or normal body weight individuals develop T2D (lean-T2D) are not yet
understood. T2D occurs when the body does not produce enough insulin, or becomes less
sensitive to its effects. Insulin acts like a key to allow sugar into cells and if someone is
overweight that key works less well. Recent research suggests that T2D in lean people should
be considered a different disease from the diabetes associated with obesity and the main
problem in lean-T2D patients may be a reduced capacity of insulin secretion. However, some
researchers argue that many seemingly thin people carry more fat than muscle, making them
trim on the outside, but fat on the inside, and they are in fact not truly lean. This implies
that just like overweight diabetics, lean diabetics also have high resistance to insulin. The
main aim of this research is to better understand the main driver of T2D in lean individuals,
as this will determine how best to treat these individuals.
There are many different types of drugs for treating T2D. Liraglutide improves insulin
secretion capacity of the pancreas. Pioglitazone reduces resistance to insulin action. The
investigators will compare the actions of these diabetes drugs on the blood supply and the
heart's energy levels in lean-T2D and obese-T2D patients. This will allow the investigators
to determine the ideal treatment strategies for improving cardiovascular health in lean-T2D
patients, and better understand the role of impaired insulin secretory capacity, insulin
resistance and excess fat deposition specifically in this group.
Description:
This is a single centre, open-label, randomized, cross-over study. Participants will attend 4
visits in total over the course of approximately 40 weeks. Two cohorts of patients will be
recruited: 28 lean-T2D patients and 28 obese-T2D patients.
Potential participants will be invited to the research centre for a screening/ baseline visit
(Visit 1). At this visit, the participants will be given the Participant Information Sheet
(PIS) to read through, and given the opportunity to ask questions. If they are interested in
participating, their consent will be taken in written form. Each participant will then have a
series of non-invasive tests. At this baseline visit, the following assessments will be done:
- Review of medical history and concomitant medications;
- Review of history of diabetes and complications;
- Review of inclusion/exclusion criteria;
- Collection of demographic data;
- Vital signs;
- Physical examination;
- Height and weight;
- Blood pressure;
- Urine pregnancy test in women of childbearing potential;
- Venepuncture (fasting sample): 20mls;
- Multiparametric MRI;
- EndoPAT testing;
- 6 minute walk test;
- 12-lead ECG;
- Randomization;
- Dispense study medication and issue patient diary; and
- Urine sample collection.
At this visit, participants will be randomized to receive either liraglutide or pioglitazone
first. Participants that are already taking certain classes of glucose-lowering medications
may be excluded from the study (see exclusion criteria for more detail). Participants will
continue to take their previously prescribed medications throughout the study.
After 16 weeks of treatment (Visit 2), participants will return to the research centre and
have the following assessments:
- Vital signs;
- Physical examination;
- Blood pressure;
- Weight;
- Venepuncture (fasting sample): 20mls;
- 12-lead ECG;
- Multiparametric MRI;
- EndoPAT testing;
- 6 minute walk test;
- Check current medication list and patient clinical status;
- Check study medication compliance (diary review); and
- Urine sample collection.
Participants will then have an 8 week washout period, in which they will take no study drug.
After these 8 weeks, they will return to the research centre (Visit 3) and have the same
assessments as listed above for Visit 2. They will start taking the second study drug for 16
weeks.
After 16 weeks, participants will attend the research centre for a final time (Visit 4) and
have the same assessments as listed above for Visit 2.
Multiparametric MRI assessments will consists of 2 parts: Magnetic Resonance Spectroscopy
(MRS): The relative concentration of phosphocreatine to ATP (PCr/ATP) by 31P-MRS and cardiac
and hepatic triglyceride content by 1H-MRS.
Collected blood will be tested for triglycerides, alanine aminotransferase, haemoglobin,
haematocrit, creatinine, estimated glomerular filtration rate, N-terminal pro-B-type
natriuretic peptide, insulin, free fatty acids, adiponectin, glucose and lipid profiles,
glutamic acid decarboxylase antibodies, and Zinc transporter 8 antibodies. Urine will be
spot-tested for albumin/ creatinine ratio.
Previous clinical studies have found an association between diabetes and impaired function of
the endothelium of blood vessels. The EndoPAT 2000 is a machine that measures endothelium
function via 2 thimble-sized sensors placed on the index fingers. This is a safe and
non-invasive way of testing the condition of the participant's blood vessels, and testing
takes about 5 minutes.
The 6 minute walk test is an exercise test that requires patients to walk along a long flat
corridor for 6 minutes to see how far they can walk at their own pace.
Liraglutide will be administered at 0.6mg once daily to start, then titrated up to 1.2mg
after 2 weeks if the participant's glucose levels permit. Participants will be trained how to
administer the injection themselves. Glucose assessments will be done after 2 weeks of
treatment with Liraglutide. Pioglitazone is taken orally. Participants will be started on
15mg once daily; this will be titrated up to 30mg after 2 weeks then to 45mg after another 2
weeks if glucose levels permit. Glucose assessments will be done 2 weeks after starting
treatment, then 4 weeks after starting treatment. Participants will be told to continue their
usual schedule of glucose monitoring at home while on the study drugs (no additional
monitoring at home will be necessary).
Participants will be given diaries to complete while they are on both drugs.
