Randomized Conversion of Calcineurin-Inhibitors(Tacrolimus to Sirolimus),6-24 Months Post Transplant Prednisone-Free Immunosuppression Regimen: Impact of Incidence of Acute Cellular Rejection,Renal Allograft Function & Lymphocytes Function
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Chicago |
| State: |
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Illinois |
| Zip Code: |
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60611 |
| Conditions: |
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Renal Transplant Rejection |
| Purpose: |
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This study is being done to investigate the impact of changing immunosuppressive medications
from tacrolimus (Prograf®) to sirolimus (Rapamune®) between 6 and 24 months post transplant.
The primary purpose of this research study is to evaluate whether the use of mycophenolate
mofetil(MMF)/Cellcept® and tacrolimus(TAC)/Prograf® (Group 1) or mycophenolate
mofetil(MMF)/Cellcept® and sirolimus/Rapamune® (Group 2) impacts the incidence of acute
cellular rejection in post kidney transplant patients. This study will examine whether
switching from tacrolimus to sirolimus will better preserve long-term kidney function.
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| Study Summary: |
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For this research study, between 6 and 24 Months post-transplant, we plan to prospectively
randomize 2:1 renal transplant patients to either:
- Substitute tacrolimus (TAC) with sirolimus and continue mycophenolate mofetil (MMF) or
- Continue with tacrolimus (TAC) and mycophenolate mofetil (MMF)
A total of 400 patients are expected to be screened for the randomization. We expect to
randomize 275 renal transplant patients into this protocol (275 donors to be recruited).
The following data will be collected at the time of randomization:
Recipient demographics: (i) age at transplantation, (ii) sex, and (iii) race.
Clinical history: (i) causes of end-stage renal disease, and (ii) past medical history.
Transplant related information: (i) donor age, (ii) cadaveric versus living kidney
transplant, (iii) histocompatibility and cross match data, (iv) viral serology, (v) history
of acute rejection and delayed graft function, (vi) use of induction therapy and
immunosuppressants, (vii) use of ACEI and/or ARB, and (viii) level of renal allograft
function-estimated GFR (e-GFR(12) using MDRD formula, proteinuria.
Peripheral blood leukocytes will be obtained from renal transplant recipients for baseline
(prior to randomization) lymphocytes functional activity and characterization of
lymphocytes subpopulations by flow cytometry analysis.
Peripheral donor leukocytes (from living donor patients) will also be obtained at the time
of randomization. These donor leukocytes will be used as stimulator cells to study the
functional activity of the recipient's lymphocytes function.
The recipients assigned to continue with tacrolimus and MMF will be routinely followed at
the outpatient Comprehensive Transplant Center (CTC) with monthly labs. In addition to labs
at baseline pre-randomization, 6, 12 and 24 Months post-randomization, peripheral blood
leukocytes will be obtained to study lymphocytes functional activity and to characterize
lymphocytes subpopulations by flow cytometry analysis.
Post randomization: The recipients assigned to switch from tacrolimus to sirolimus and
continue with MMF will be routinely followed at the CTC with monthly labs. During the period
of conversion from tacrolimus to sirolimus, weekly labs will be obtained to monitor renal
function and bone marrow function. In addition to labs at baseline pre-randomization, 6, 12
and 24 Months post-randomization, peripheral blood leukocytes will be obtained to study
lymphocytes functional activity to characterize lymphocytes subpopulations by flow cytometry
analysis. Urine will be collected to assess tubular toxicity by evaluating urinary
biomarkers.
Both groups of patients will be followed for 2 years post-randomization. In addition to
monitoring renal allograft function, we will evaluate the incidence of acute rejection,
patient and graft survival, impact of CI conversion on the lipid profile, incidence of
hypertension, malignancies, opportunistic infections, and post-transplant DM. For those
willing to undergo an optional kidney biopsy, one will be performed at the end of the second
year in order to evaluate renal allograft pathology and renal allograft tissue gene
expression profiles of the two groups.
With the peripheral leukocytes obtained at baseline prior to randomization and at 6, 12 and
24 Months post-randomization, we will investigate possible modifications of lymphocytes
function and the lymphocytes subpopulations that might have occurred as a consequence of the
switch from tacrolimus to sirolimus.
Obtaining renal allograft tissue samples at 24 months post randomization can have potential
important ramifications to help explain the mechanisms of fibrosis and tubular atrophy
typically associated with CI and the role of CI elimination with the substitution of SRL.
All data will then be analyzed comparing gene expression profiles of peripheral blood
(Paxgene tubes are routinely collected at the different time points as part of the original
study). Based on power analysis, we will perform 24 months post randomization biopsies in
70% of the total subjects enrolled in the study (approximately 46 subjects from the
tacrolimus/MMF group and approximately 93 subjects from the sirolimus/MMF group).
We plan to obtain renal allograft biopsies at 24 Months for those that consent for this
additional biopsy. This will be compared to the standard of care 12 months post-transplant
biopsy to allow us to address the effect of immunosuppressive modifications on renal
allograft pathology at 24 months post randomization. Renal allograft biopsies will also be
stored in RNA later to further extend our knowledge on the effect of CI free
immunosuppression on gene expression profiles.
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| Criteria: |
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Inclusion Criteria:
1. Subjects should be adults ≥ 18- ≤ 70 years of age
2. Subjects can be either gender or of any ethnic background
3. Subjects should be single organ recipients (kidney only)
4. Subjects must be able to understand the protocol and provide informed consent.
Exclusion Criteria:
1. Subjects with ESRD secondary to primary FSGS (focal segmental glomerulonephritis).
2. Inability to comply with study procedures
3. Inability to sign the informed consent
4. Subjects with a significant or active infection
5. Subjects who are pregnant or nursing females
6. Subjects with a history of severe hyperlipidemia not controlled with statins,
patients with at total cholesterol of > 400 mg/dl
7. Subjects with a platelet count <100,000mm3 WBC< 2,000mm3
8. Subjects with severe proteinuria at the time of randomization (>2gm/day)
9. Subjects with more then 2 episodes of acute cellular rejection post transplantation
will be excluded from this study
10. An estimated GFR<40 cc/min
11. A history of malignancy during the post-transplant period (other than treated basal
cell cancer and/or squamous cell cancer)
12. Subjects, who, due to the existence of a surgical, medical or psychiatric condition,
other than the current transplant, which in the opinion of the investigator,
precludes enrollment into this trial
13. A history of ACR during the most recent previous 3 months prior to randomization
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| NCT ID: |
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NCT00866879 |
| Primary Contact: |
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Principal Investigator
Lorenzo Gallon, MD
Northwestern Univesity, Northwestern Memorial Hospital, Northwestern Medical Faculty Foundation
Farida Siddiqui, CCRP
Phone: 312-694-0242
Email: f-siddiqui@northwestern.edu
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| Backup Contact: |
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N/A |
| Location Contact: |
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Chicago, Illinois 60611
United States
There is no listed contact information for this specific location.
Site Status: Recruiting |
| Data Source: |
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ClinicalTrials.gov |
| Date Processed: |
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May 24, 2013 |
| Modifications to this listing: |
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