Study Results
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Basic Information
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COMPLETED
PHASE4
18 participants
INTERVENTIONAL
2008-03-31
2011-11-30
Brief Summary
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Randomized, investigator-blinded cross-over studies will be carried out, studying 10 healthy subjects and 10 hemodialysis patients. Each participant will receive treatment with CsA, Tac and placebo respectively in a random order. The results will be of relevance to the choice and monitoring of immunosuppressive regimens in kidney transplant recipients as well as the development of better treatment modalities for diabetes.
Detailed Description
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To or knowledge, comparison of the diabetogenic effects of CsA and Tac, without concomitant corticosteroids, has never been investigated using the gold standard to estimate insulin sensitivity; a hyperinsulinemic euglycemic glucose clamp (HEGC).
Hypotheses: CsA and Tac are able to induce diabetes, by exerting acute and chronic effects on pancreas beta-cell performance and insulin sensitivity.
The hypothesized effects will be investigated during following studies:
1. Acute effect in 10 healthy subjects undergoing HEGC
2. Chronic effect in 10 pre-transplant uremic patients undergoing HEGC
Methods: The studies are randomized, double-blinded (Study 1) and investigator blinded (Study 2) cross-over designs. Each study subject participates in three experimental study days with an interval of 4-6 weeks. A HEGC is carried out on the study days, where treatment includes CsA, Tac and placebo respectively in random order. Following an overnight fast the healthy subject / uremic patient arrives in the research laboratory, where a catheter is implanted in each arm for blood sampling and infusion purposes.
Pulse induction: Glucose 6 mg/kg/min is infused every 10 minutes followed by a 9 minute pause. From 30 to 90 min blood is drawn every minute for insulin and every 10th minute for glucose measurements.
First phase insulin secretion: After 120 minutes glucose 0.3 g/kg (maximally 25 g) is infused over 2 min and the catheter is flushed with 50 ml of isotonic saline. Insulin, glucose and c-peptide are measured with a few minutes intervals.
Insulin infusion/HEGC: 1.0 mU/kg/min insulin infusion is initiated at the 165th minute and blood glucose levels are kept at 5.0 mmol/L, using variable infusion of a 20% glucose dilution throughout the following 120 minutes. The final 30 min of the clamp is considered the hyperinsulinaemic steady state period. Aside from glucose, insulin and other endocrinological parameters, measurements of drug concentration and CaN will also be performed.
Perspectives: The studies are expected to give valuable insight into the diabetogenic effects of CI, and to show whether or not CsA and Tac are comparable in their Diabetogenicity. The results will be of relevance to the choice and monitoring of immunosuppressive regimens in kidney transplant recipients as well as the development of better treatment modalities for diabetes.
Conditions
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Study Design
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RANDOMIZED
CROSSOVER
TREATMENT
TRIPLE
Study Groups
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CsA
Cyclosporine
cyclosporine
For Healthy volunteers (study 1) and Dialysis patients (study 2): Single intravenous infusion of 0.155 mg/kg over a maximum duration of 5 hours.
For Dialysis Patients (study 2): Oral intake of 4 mg/kg 2 times daily for 8-11 days.
Tac
Tacrolimus
tacrolimus
For Healthy volunteers (study 1) and Dialysis patients (study 2): Single intravenous infusion of 0.0012 mg/kg over a maximum duration of 5 hours.
For Dialysis Patients (study 2): Oral intake of 0.1 mg/kg 2 times daily for 8-11 days.
Placebo
placebo/saline
Capsules and isotonic saline
For Healthy volunteers (study 1) and Dialysis patients (study 2): Single intravenous infusion of 0.06 ml/kg isotonic saline over a maximum duration of 5 hours.
For Dialysis patients (study 2): Placebo capsules 2 times daily for 8-11 days.
Interventions
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cyclosporine
For Healthy volunteers (study 1) and Dialysis patients (study 2): Single intravenous infusion of 0.155 mg/kg over a maximum duration of 5 hours.
For Dialysis Patients (study 2): Oral intake of 4 mg/kg 2 times daily for 8-11 days.
tacrolimus
For Healthy volunteers (study 1) and Dialysis patients (study 2): Single intravenous infusion of 0.0012 mg/kg over a maximum duration of 5 hours.
For Dialysis Patients (study 2): Oral intake of 0.1 mg/kg 2 times daily for 8-11 days.
Capsules and isotonic saline
For Healthy volunteers (study 1) and Dialysis patients (study 2): Single intravenous infusion of 0.06 ml/kg isotonic saline over a maximum duration of 5 hours.
For Dialysis patients (study 2): Placebo capsules 2 times daily for 8-11 days.
Other Intervention Names
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Eligibility Criteria
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Inclusion Criteria
1. Men.
2. Age between 18 years and 50 years. Upper limit can be +2 years if approved by main investigator.
3. Normal OGTT (0 and 120 min test).
4. Body mass index (BMI) 20 - 30 kg/m2. Allowed variations are 5% from the upper and lower limit.
5. Normal serum creatinine and ionisized calcium. Allowed variations are 20% from the upper and lower limit of the normal value for creatinine and 5% for calcium.
6. Normal urine stix
7. Written consent to participate.
Hemodialysis Patients (study 2):
1. Age between 18 years and 70 years. Upper limit can be +2 years if approved by main investigator.
2. BMI \< 30 kg/m2. Allowed variations are 5% over the upper limit.
3. On the waiting-list for a kidney transplant.
4. Haemodialysis candidate.
5. Anti-conceptive treatment (contraceptive pill/intrauterine device/patch/ring/ implant/injectable contraceptive) if the patient is a fertile woman.
6. Written consent to participate. -
Exclusion Criteria
1. Anaemia with haemoglobin levels \< 7 mmol/L
2. Participation in any other clinical trial.
3. Subjects who cannot adhere to test conditions.
4. Anamnesis of clinically significant disease, such as:
* liver disease
* kidney disease,
* neurological disease
* gastrointestinal disease
* haematological disease
* endocrine disease
* lung disease
* cardiac disease
5. Drug or alcohol abuse, which would render the subject unfit according to the main investigator.
6. Blood donation 1 month prior to the study day
7. Patients with established allergy against CI or other medical products, which might pose a risk if they participated in this study.
8. Use of prescription drugs within one month prior to the study days, unless they are clinically insignificant according to the main investigator.
9. Smoking 8 hours prior to the study day
10. Vigorous exercise 30 minutes prior to the study day.
Hemodialysis Patients (study 2):
1. Peritoneal dialysis.
2. Anaemia with haemoglobin levels \< 6 mmol/L.
3. Participation in any other clinical trial.
4. Treatment with corticosteroids, CsA or Tac.
5. Patients who cannot adhere to test conditions.
6. Patients with established allergy against CI or other medical product, which might pose a risk if they participated in this study.
7. Drug or alcohol abuse, which would render the subject unfit according to the main investigator.
8. Anamnesis of current diabetes and/or intake of anti-diabetic medication.
9. Malignancy.
10. Uncontrolled infection.
11. Uncontrolled hypertension.
12. Smoking 8 hours prior to the study day.
13. Vigorous exercise 30 minutes prior to the study day
\-
18 Years
70 Years
ALL
Yes
Sponsors
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University of Aarhus
OTHER
Responsible Party
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Principal Investigators
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Lara Aygen Øzbay, MD
Role: PRINCIPAL_INVESTIGATOR
Aarhus University Hospital Skejby
Locations
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Department of Nephrology, Aarhus University Hospital, Skejby
Aarhus, Jutland, Denmark
Countries
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References
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Ozbay LA, Stubbe J, Jespersen B, Jensen BL. The effects of calcineurin inhibitors on prostanoid synthesis: a randomized cross-over study in healthy humans. Transpl Int. 2013 Feb;26(2):131-7. doi: 10.1111/tri.12004. Epub 2012 Nov 29.
Ozbay LA, Moller N, Juhl C, Bjerre M, Carstens J, Rungby J, Jorgensen KA. The impact of calcineurin inhibitors on insulin sensitivity and insulin secretion: a randomized crossover trial in uraemic patients. Diabet Med. 2012 Dec;29(12):e440-4. doi: 10.1111/dme.12028.
Other Identifiers
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M-20080060
Identifier Type: -
Identifier Source: org_study_id