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Clinical Trial Details — Status: Terminated

Administrative data

NCT number NCT01213394
Other study ID # ML25073
Secondary ID
Status Terminated
Phase Phase 3
First received September 28, 2010
Last updated April 18, 2012
Start date October 2010
Est. completion date December 2011

Study information

Verified date April 2012
Source St. Michael's Hospital, Toronto
Contact n/a
Is FDA regulated No
Health authority Canada: Health Canada
Study type Interventional

Clinical Trial Summary

The purpose of this research study is to determine if adding or increasing the dose of CellCept while lowering the dose of tacrolimus (Prograf or Advagraf) or cyclosporine (Neoral), and/or steroids can reduce the likelihood of developing coronary heart disease in the next 10 years.

The investigators will calculate the change in risk of developing coronary heart disease using the Framingham score. The Framingham score is a mathematical equation that includes the following information: Age, Gender, Diabetes status, Smoking status, Lipids, Blood Pressure. The Framingham score estimates how likely it is that someone will develop coronary heart disease over the next 10 years.


Description:

Kidney transplant recipients are required to take medications called immunosuppressants to lower their immune systems to help protect the donated kidney. The medications have improved over the years and as a result the donated kidneys are generally working longer. This allows the Transplant Team to focus more on the long term complications of kidney transplantation such as cardiovascular disease.

There have been few prospective (looking forward) research studies looking at kidney transplant recipient cardiovascular risk factors after transplant.

We know that immunosuppressive medications have a number of serious side effects that can increase cardiovascular disease risk factors such as high blood pressure, high lipids (fats in the blood), and high blood sugar. Medications such as tacrolimus, cyclosporine and prednisone work well to protect the donated kidney but are also known to increase the risk of developing or worsening cardiovascular disease.

CellCept is another type of immunosuppressive agent. CellCept is not associated as much with the risk of developing cardiovascular disease.

This is a pilot study being done to collect information about cardiovascular risk factors in kidney transplant recipients and to see if adjusting the immunosuppressive medications can help to lower the overall risk for developing heart disease in the future.

This research study plans to enroll 45 participants from 2 different transplant centres in Canada: St. Michael's Hospital in Toronto and St. Paul's Hospital in Saskatoon. The study duration is approximately 7 months per participant. The study will be looking for participants who are 30 years of age or older and who are at least 6 months after the transplant operation.


Recruitment information / eligibility

Status Terminated
Enrollment 2
Est. completion date December 2011
Est. primary completion date October 2011
Accepts healthy volunteers No
Gender Both
Age group 30 Years and older
Eligibility Inclusion Criteria:

1. Renal transplant recipients who are = 6 months post-day of transplant surgery.

2. Single organ kidney recipient (may be for first or repeat transplant).

3. Age = 30 years of age as of the Day 0 visit.

4. Immunosuppressive regimen consisting of a CNI (cyclosporine [CsA, Neoral] or tacrolimus [TAC, Prograf or Advagraf], corticosteroids and either MMF (CellCept), EC-MPS (Myfortic), AZA (Imuran) or SRL (Rapamune) at the baseline visit. Patients are to be maintained on the same dose(s) for at least 4 weeks prior to study enrolment.

5. If the patient is taking an MPA immunosuppressant at the time of the screening visit, the MMF (CellCept) dose must be = 1500 mg/day; or the EC-MPS (Myfortic) dose must be = 1080 mg/day.

6. Framingham risk factor score that exceeds the low comparative 10-year CHD risk, based on age and gender.

7. Presence of at least one established CV risk factor at baseline warranting modification of the immunosuppressive regimen including:

- Hypertension: Blood pressure = 140 mmHg systolic and/or = 90 mmHg diastolic and/or requiring = 1 antihypertensive medication.

- Diabetes mellitus: Established diabetes requiring treatment with oral hypoglycemic agents or insulin, or known IFG or IGT based on 75-g oral glucose tolerance testing (2003 Canadian Diabetes Association criteria).

- Hyperlipidemia: TC = 5.2 mmol/L, or LDL-C = 2.6 mmol/L, or TG = 1.7 mmol/L, or TC:HDL = 4 and/or requiring = 1 anti-hyperlipidemia agent.

8. Willingness and ability to complete protocol requirements.

9. Written informed consent.

Exclusion Criteria:

1. Contraindication to receiving MMF (CellCept) or increasing CellCept dose.

2. Clinically suspected acute rejection (AR) or BPAR within 3 months prior to the baseline visit.

3. Proteinuria = 1 g/24 hours

4. Treatment with AZA (Imuran), EC-MPS (Myfortic) or SRL (Rapamune) and patient or physician decision not to discontinue these agents and switch to MMF (CellCept) at the time of randomization.

5. MDRD (4-variable) eGFR < 15 mL/min/1.73 m2

6. Patients who currently exceed thresholds for plasma glucose, cholesterol or blood pressure. Patients may be re-considered 1 month after the treatment is in place and no further therapeutic changes are anticipated.

7. Patients who require changes to their blood pressure, blood sugar or blood lipid management between the Screening Visit and Day 0. Patients may be re-considered 1 month after the adjusted treatment is in place and no further therapeutic changes are anticipated.

8. Pregnancy, lactation or (for women of childbearing potential) inability or decision not to use a reliable method of contraception for the entire study duration.

9. Active infection requiring treatment.

10. Treatment with unlicensed investigational drugs, devices or other prohibited medications - see Section 4.4.1

11. Participation in any other interventional clinical trial during the previous 4 weeks or during this trial.

12. History of malignancy, other than non-melanoma skin cancer that has been totally excised and has not recurred for >2 years.

13. History of psychological illness or condition that could interfere with the patient's ability to understand or comply with the study requirements.

14. Presence of other significant diseases or issues which, in the opinion of the sponsor-investigator, may:

- Put the patient at risk as a result of study participation

- Influence the study result

- Affect the patient's ability to participate in the study

- Require a change in immunosuppression medication used or a dose change within the next 6 months (unstable renal function, gout that may require treatment with prednisone, etc)

- Reduce life expectancy. Examples include but are not limited to history of noncompliance and transportation issues that could affect a participant's ability to successfully complete the study requirements. Inability or refusal to provide blood samples, end-stage disease of organs such as lung, liver or heart.

15. Exclusion of patients who are hypersensitive to CellCept (mycophenolate mofetil), mycophenolic acid or any component of the drug).

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Prevention


Related Conditions & MeSH terms


Intervention

Drug:
mycophenolate mofetil
Introduction of CellCept or increase in the dose of CellCept to a maximum of 2 g/day. In patients not already receiving CellCept, azathioprine (AZA), enteric-coated mycophenolate sodium (EC-MPS) or sirolimus (SRL) will be discontinued and replaced by CellCept in divided doses to a maximum of 2 g/day. CNI doses will be reduced to conform to the target trough levels in the low-dose CNI arms of the ELITE-Symphony study +/- steroid dose reduction. Any CNI dose change will require measurement of CNI trough levels at 7 days post dose change +/- 3 days. Target CNI trough levels in the Symphony study: Low-dose CsA: Initial oral dose of 1-2 mg/kg bid, to achieve a target trough level of 50-100 ng/mL. Low-dose TAC: Initial oral dose of 0.1 mg/kg/day divided into two doses* with a target trough level of 3-7 ng/mL (*Advagraf may also be used at a dose of 0.1 mg/kg once daily with a target trough level of 3-7 ng/mL)
Other:
standard immunosuppression
Current immunosuppressive therapy will be maintained throughout the study unless a change is required for safety reasons.

Locations

Country Name City State
Canada St. Michael's Hospital Toronto Ontario

Sponsors (2)

Lead Sponsor Collaborator
Ramesh Prasad Hoffmann-La Roche

Country where clinical trial is conducted

Canada, 

Outcome

Type Measure Description Time frame Safety issue
Primary The change in the Framingham 10-yr age and gender adjusted score for coronary heart disease from baseline to Month 6 Baseline to Month 6 No
Primary The incidence of a composite of acute rejection (clinically suspected and biopsy-proven), graft loss or patient death. Month 6 Yes
Secondary Framingham point total Change in Framingham point total from baseline to month 6 Baseline to Month 6 No
Secondary Day and night blood pressure Change in day and night blood pressure (defined by awake and sleep times) measured by 24-hour ambulatory blood pressure monitoring (ABPM) from baseline to month 6 Baseline to Month 6 No
Secondary Glucose metabolism Change in glucose metabolism, based on HbA1C levels in patients with and without diabetes, and the prevalence of impaired fasting glucose (IFG) and impaired glucose intolerance (IGT) in patients without overt diabetes from baseline/randomization to month 6. Baseline to Month 6 No
Secondary Lipid metabolism Change in lipid metabolism, measured by the fasting levels of total cholesterol (TC), high-density lipoprotein cholesterol (HDL-C), low-density lipoprotein cholesterol (LDL-C) and triglycerides (TG)and ratio of TC to HDL-C from baseline/randomization to month 6 Baseline to Month 6 No
Secondary Change in renal function Change in renal function from baseline/randomization to month 6 as measured by serum creatinine, estimated glomerular filtration rate, (MDRD 4-variable equation), change in eGFR slope, change in chronic kidney disease (CKD), 24-hr urine creatinine clearance and protein/albumin excretion Baseline to Month 6 No
Secondary Adverse cardiovascular events Proportion of patients who experience any adverse cardiovascular event such as myocardial infarction (MI), percutaneous coronary intervention (PCI), coronary artery bypass grafting (CABG), fatal and non-fatal cerebrovascular events (including fatal or non-fatal stroke, transient ischemic attack, reversible ischemic neurological deficit and subarachnoid hemorrhage). Cardiovascular events will be adjudicated by a cardiologist blinded to treatment assignment. Month 6 No
Secondary Highly-sensitive C-reactive protein (CRP) level Change in highly-sensitive CRP level between randomization and month 6. Randomization to Month 6 No
Secondary Change in other biomarkers of cardiovascular risk Change in other biomarkers of cardiovascular risk between randomization and month 6: human adiponectin (including its high molecular weight isoform), uric acid, early morning urine albumin-to-creatinine ratio, B-type (brain) natriuretic peptide (BNP), fibrinogen, D-dimer (fibrin degradation fragment), advanced glycosylation endproduct (AGE), paraoxonase B, cystatin C, insulin, proinsulin, malondialdehyde (MDA), protein carbonyl, glutathione reductase/total and apolipoprotein A1, B and Lp(a). Randomization to Month 6 No
Secondary Incidence of MMF-attributable adverse events Incidence of MMF-attributable adverse events including gastrointestinal toxicities, thrombocytopenia, leucopenia and anemia. Month 6 Yes
Secondary Additional treatment with cardiovascular co-interventions Requirements for additional treatment with cardiovascular co-interventions - as per guideline documents. Month 6 Yes
Secondary Opportunistic infections Incidence of opportunistic infections Month 6 Yes
Secondary Malignancies Incidence of malignancies Month 6 Yes
Secondary Adverse events All adverse events (AEs), including clinically significant abnormalities of clinical and laboratory parameters will be captured. Summary statistics will be created for all adverse events and will be summarized by treatment group, by relation to study treatment and seriousness of the event. Month 6 Yes
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