Liver Diseases Clinical Trial
Official title:
Study of ATEGE-Fresenius Induction in Liver Transplantation Followed by Tacrolimus Weaning.
This is a randomized, controlled trial in liver transplantation in which conventional immunosuppressive treatment will be compared with a therapeutic strategy consisting in pre-transplant antibody-mediated T cell depletion followed by reduced calcineurin inhibitor usage. The working hypothesis is that antibody induction followed by calcineurin inhibitor minimization may promote development of tolerogenic mechanisms allowing the eventual withdrawal of all immunosuppressive therapy.
This is an open-label randomised controlled study in which patients will be randomised
according to a 1:1 ratio to receive conventional immunosuppressive treatment or induction
treatment plus reduced tacrolimus dosage. All transplanted patients enrolled in the study
will be followed during 12 months and evaluated according to an intention-to-treat approach.
- Specific Aim 1: To determine the proportion of liver recipients in whom tacrolimus
usage can be significantly reduced 1 year after transplantation. Patients will be
considered as successfully receiving a reduced tacrolimus regimen if this drug is given
as a single dose every other day, or at the most administered as a single dose daily
with trough levels < 5ng/mL.
- Specific Aim 2: To determine the effect of induction treatment plus minimized
immunosuppression on graft and patient survival.
- Specific Aim 3: To determine the impact of induction treatment plus minimized
immunosuppression on the development of: acute and chronic allograft rejection,
hepatitis C virus graft recurrence, opportunistic infections, bone fractures, kidney
failure, tacrolimus-related neurotoxicity, dyslipidemia and arterial hypertension.
- Specific Aim 4: To establish whether the use of ATG induction followed by reduced doses
of tacrolimus differentially affects anti-donor immune responses and/or promotes the
development of T cell dependent immunoregulatory networks.
- Conventional immunosuppressive protocol:
1. Methylprednisolone iv 500 mg before laparotomy, and 500 mg at the time of
reperfusion.
2. Methylprednisolone iv according to the following schedule: postoperative day 1 200
mg, day 2 160mg, day 3 120 mg, day 4 80 mg, day 5 40 mg, and thereafter 20 mg oral
prednisone.
3. Oral tacrolimus q12h starting on postoperative day 1 in order to reach trough drug
levels between 10 and 15 ng/mL. These levels will be maintained in this range
during the first month after transplantation. Subsequently, tacrolimus levels will
be gradually reduced as follows: : month 1-3: 8-15 ng/ml; month 4-12: 7-12 ng/ml;
afterwards: 5-10 ng/ml.
4. Progressive prednisone withdrawal between month 6 and 9 after transplantation.
5. Treatment of acute rejection episodes: according to our conventional clinical
protocol. All efforts must be done in order to histologically document the
rejection episode. Hence, empirical treatment should be avoided if possible.
- Induction protocol:
1. ATG-Fresenius 9mg/kg pre-transplantation, preceded by administration of 500 mg iv
methylprednisolone. Infusion of ATG-F will be started whenever the surgeon
confirms the suitability of the graft, and will take place during 6 hours.
2. Oral tacrolimus q12h, starting on postoperative day 1 at the required dosages in
order to reach through drug levels between 5 and 12 ng/mL
3. Reduction of tacrolimus dosages starting 3 months after transplantation in stable
patients with no evidences of graft rejection in the previous 60 days, and
according to the following protocol:
- posttransplant month 3: 1 dose per day
- posttransplant month 6: 1 dose every 48 hours
- posttransplant month 9: ½ dose every 48 hours
- posttransplant month 12: evaluate the possibility of complete drug withdrawal
or alternatively establish the optimal maintenance dose.
4. Treatment of acute rejection episodes: mild to moderate acute rejection episodes:
re-start 1-2 daily doses of tacrolimus. Severe acute rejection episodes or those
mild to moderate episodes that do not improve after 10 days of treatment: 1-2
daily doses of tacrolimus plus methylprednisolone 0.5-1 g for 3 days. Resolution
of the rejection episode will be followed by resumption of the above mentioned
protocol. If a new rejection episode takes place, after treatment of the acute
episode no further attempts to reduce tacrolimus dosages will be attempted. In all
cases rejection will be confirmed by liver biopsy.
5. Patients suffering from hepatitis C virus infection will be treated as above,
unless alpha-interferon treatment is considered. In this case, daily tacrolimus
will be administered.
6. All patients will receive CMV prophylaxis with iv ganciclovir for 14 days and oral
valganciclovir to complete 3 months after transplantation.
- Sample collection during the study period
In addition to routine diagnostic tests, all enrolled patients will undergo the following
procedures:
- Cryopreservation of donor spleen cells to measure anti-donor immune responses.
- HCV viral load quantification pre-transplantation and at post-transplant months 1, 6
and 12.
- All patients will undergo liver biopsy 1 year after transplantation and yearly
thereafter. In addition, HCV positive patients will be undergo liver biopsy 3 months
after transplantation. A portion of all liver biopsies will be cryopreserved for gene
expression studies.
- Anti-donor and anti-HCV T cell immune responses will be quantified before
transplantation, and 6 and 12 months after transplantation by gamma-interferon ELISpot
assay.
- Peripheral blood mononuclear cells will be harvested and cryopreserved before
transplantation, 6 months and 12 months after transplantation to perform gene
expression and flow cytometry studies.
- A sample of recipient DNA will be cryopreserved to perform DNA polymorphism studies.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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