Immunosuppression Clinical Trial
Official title:
Thymoglobulin Induction Therapy With Minimal Immunosuppression and Evaluation of Allograft Status by Biopsy and mRNA Profiles (TIMELY Study)
Tacrolimus (Prograf) is a medication that is commonly used in patients who receive a kidney transplant. It is considered to be one of the most important medications that prevent rejection of the transplant kidney by suppressing the immune system. Although tacrolimus is good at preventing rejection, it does have some unwanted side effects. These side effects include high blood pressure, increase in blood sugar, headache, and tremor. In addition, tacrolimus causes some damage to the transplant kidney over time, by causing healthy tissue to turn into scar tissue that does not function as well as healthy tissue. Therefore, kidney function may be reduced over time. In the first three months after kidney transplant, Prograf levels are kept between 8 to 10 ng/mL. This study will compare two groups of patients that will both have their tacrolimus dose reduced slowly over three months to prevent rejection while decreasing the risk of causing toxic effects to the kidney. One group will have their Prograf levels kept between 6 and 8 ng/mL, while the second group will have their levels kept between 3 and 5 ng/mL. We will then compare the two groups to see if there are any differences in their kidney function over time.
The objective of this study is to assess the safety and efficacy of an
immunosuppression-minimizing regimen consisting initially of Thymoglobulin induction in
combination with tacrolimus, mycophenolate mofetil, and rapid steroid withdrawal. The
protocol will minimize long-term calcineurin inhibitor exposure and toxicity by weaning
tacrolimus starting at 3 months after transplantation. Patients will be eligible to
participate in this study only if they have already consented to participate in another study
entitled "The use of urinary PCR test to help detect rejection in kidney transplant
patients". In "The use of urinary PCR test to help detect rejection in kidney transplant
patients", kidney allograft status (ie. whether or not there is any immunologic activity in
the transplant kidney)is characterized with the use of protocol biopsies, diagnostic
biopsies, and urinary PCR profiles. At 3 months after transplant, these patients are on an
immunosuppression regimen consisting of tacrolimus (Prograf) and mycophenolate mofetil
(CellCept). Prograf dosing is managed through the measurement of trough levels. For the first
3 months after transplant, patients are maintained at a trough level between 8 to 10 ng/ml.
After 3 months, this target level is lowered in order to minimize long-term exposure to
immunosuppressive agents. However, there is no consensus as to what the proper level should
be after the first 3 months. Therefore, this study will randomize patients to 2 groups, one
group will have their trough level targeted between 6 to 8 ng/mL while the other group will
have their trough targeted between 3 and 5 ng/mL. By doing this study, we hope to determine
which trough level is best, both for protecting the patient from rejection and protecting the
patient from the adverse effects of the immunosuppressive medications.
At New York Weill Cornell Center, we are in a unique position to attempt immunosuppression
minimization due to our ability to non-invasively monitor patients using their urine.
Previous investigations performed at this center have demonstrated the diagnostic accuracy of
mRNA levels of cytotoxic attack molecules in urinary cells. Preliminary data has shown that
during acute rejection, Granzyme B and Perforin are strongly expressed in the urine. The
sensitivity of the uPCR test was 88% with a specificity of 79%. All kidney transplant
recipients at our center are invited to participate in the research study entitled "The use
of urinary PCR test to help detect rejection in kidney transplant patients". In this
protocol, serial analyses of urinary cells are performed to determine 1) if changes in mRNA
levels will predict clinical acute rejection and 2) if these levels correlate with the
presence of subclinical acute rejection. Kidney transplant recipients have serial urinary PCR
measurements. In addition, patients undergo protocol biopsies of the transplant kidney at 3,
15, and 36 months after transplant. The biopsies help to show the correlation between the PCR
results and the pathology of the kidney. It may also serve to detect rejection when the blood
tests or urinary PCR do not show it. In a small subset of patients, urinary gene expression
profile of cytotoxic attack molecules was able to predict acute rejection prior to clinical
diagnosis by renal allograft biopsy.
Because we have the ability to monitor our transplant recipients using the urinary PCR
protocol, we can safely minimize tacrolimus exposure over time by monitoring patients
non-invasively on a real-time basis. Minimization of immunosuppression over time in a kidney
transplant recipient is important in order to prevent or minimize some of the leading causes
of kidney graft loss (defined as return to dialysis). Although immunosuppressive medications
are excellent at preventing rejection, they do have detrimental effects on the cardiovascular
system as well as to the transplant kidney itself. One major cause of kidney graft loss today
is chronic allograft nephropathy (CAN). Formerly known as "chronic rejection", CAN has been
described as the progressive decline in allograft function that occurs months or years after
transplantation, and it is the second leading cause of kidney graft loss. Biopsies of kidney
allografts with CAN may show inflammation, fibrosis, glomerulosclerosis, tubular atrophy, and
vascular smooth muscle proliferation. The scarring and fibrosis associated with CAN is
generally irreversible. A new goal within the modern transplant arena is to prevent CAN from
occurring by:
1. decreasing early acute rejection episodes
2. decreasing calcineurin inhibitor-related nephrotoxicity
With the use of modern immunosuppressive agents and induction therapy, we have already
decreased early acute rejection episodes significantly. At this time, we now want to begin to
study the potentially beneficial effects that calcineurin inhibitor withdrawal may have on
kidney function as well as long-term graft survival.
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