Chronic Kidney Failure Clinical Trial
Official title:
CNI Transient Replacement by Belatacept From 3 to 12 Months Post Transplantation in Patients With Early Graft Dysfunction
Calcineurin inhibitors (CNI) remain the standard treatment in renal transplantation to prevent rejection. Currently the main limitation of kidney transplantation is the occurrence of chronic graft dysfunction due to the CNI nephrotoxicity. Thus, strategies to minimize or stop CNI have been developed as belatacept, a fusion protein (CTLA4-Ig) blocking the ligand of the main CD28 costimulatory molecule. In the original phase III trial, used de novo in combination with MMF (without CNI) belatacept allowed to obtain a better renal function as soon as 1 year and a better graft and patient survival after 7 years. Despite these excellent results, belatacept has not become the gold standard due to a higher incidence of early rejection. In addition, belatacept is not covered by the french social security policy, because benefits are considered insufficient with respect to the cost. Patients with poor early graft function are a preferred indication of belatacept. It is then used instead of CNI at 3 months post-transplant allowing to improve kidney function without over-risk of rejection. Currently after conversion, belatacept is maintained indefinitely due to the supposed CNI chronic nephrotoxicity. However this one is more and more questionable. Thus, the investigators assume that in patients with poor function at 3 months posttransplantation the belatacept's benefit could be obtained by a transient replacement of CNI by belatacept from 3 to 12 months post-transplantation. It is the feasibility of this strategy and its medico-economic impact that the investigators wish to study.
The standard maintenance regimen in renal transplantation combines calcineurin inhibitor
(CNI: ciclosporin or tacrolimus) and anti-metabolite drugs (mycophenolate mofetil (MMF) or
mycophenolic acid (MPA)). CNI in the 1980s made kidney transplantation possible by
drastically reducing acute rejection rates in the first year. Currently the main limitation
of kidney transplantation is the occurrence of chronic graft dysfunction. While half of
patients die with a functional graft, the other half return to dialysis and require
retransplantation. Paradoxically, CNI has been identified as a leading cause of chronic graft
dysfunction. Indeed, these molecules are nephrotoxic both : acutely and transitory due to a
vasoconstrictor effect that modulates intra-renal hemodynamic and chronically due to
extensive fibrosis. In the late 1990s, with the development of a new class of
immunosuppressants, mammilian target of rapamycin (mTor) inhibitors (sirolimus and
everolimus), CNI-free protocols were developed. The results were disappointing due in part to
the undesirable effects of these treatments and secondly to the occurence of chronic
rejections related to the appearance of Donor Specific Antibody (DSA) antibodies.
Finally in the mid-2000s belatacept is a fusion protein (CTLA4-Ig) blocking the ligands of
the main costimulatory molecule (CD28) emerged. In the Phase III princeps assay (BENEFIT),
this molecule was used as a maintenance treatment following transplantation (de novo) in
combination with MMF (without CNI). Compared to the control group with CNI, patients
receiving belatacept had better renal function from 1 year and after 7 years survival (graft
and patient) were better. These benefits were attributed, on the one hand, to the absence of
CNI and, on the other hand, to a very good control of the alloimmune response demonstrated by
a lower incidence of DSA in the belatacept group.
Despite these excellent results, belatacept has not become the gold standard in renal
transplantation for two main reasons. First, when it is used de novo (as in BENEFIT), there
is a significant incidence of early rejection, known as "costimulation blockade resistant".
The second issue is medico-economic. Indeed, to date and despite the accumulation of
favorable data, in France and in most countries, belatacept has marketing authorization but
is not supported by social security policy due to benefits regarded as insufficient with
respect to the cost (related to the IV administration requiring hospital environment every
month).
Consequently, it is important to precise which recipients may benefit more from this
molecule. Patients, often elderly, with poor early function of the graft due to the poor
quality of a marginal / "extended criteria" donor, are a good indication of belatacept not
used de novo but after 3 months instead of CNI. This conversion most often allows to
significantly improve the renal function of these patients to a much more acceptable level
which remains stable beyond and without cost in terms of rejection (probably because of the
time interval with the transplant). In this situation, several series reported success rates
ranging from 80 to 100% with a rejection incidence between 0 and 20%. Failures are most often
due to patients with non-primary graft function.
Currently after the conversion, belatacept is always maintained indefinitely most often in
association with MMF. This usage generates significant costs and in fact, limits the access
of belatacept for other patients. This practice is based on the dominant idea that chronic
nephrotoxicity of CNI is the cause of chronic graft dysfunction.
However, while reversible acute toxicity, mediated by hemodynamic changes in intra-renal
vascularization, is undeniable, the importance and even the reality of chronic, cumulative,
irreversible CNI toxicity has been questioned during the last decade, while the importance of
chronic anti-donor antibody (DSA) rejection to explain chronic graft dysfunction was
demonstrated. The chronic toxicity of CNI is probable when high doses are necessary to
prevent rejection during the first year but uncertain beyond.
Thus, the investigators assume that in patients with poor graft function at 3 months
post-transplantation most of the benefit of belatacept could be obtained by a transient
replacement of CNI from 3 to 12 months post-transplantation.
Indeed, in these often elderly patients, who have most often received an "extended criteria"
graft (derived from a marginal donor), presenting chronic lesions, CNI-induced intra-renal
vasoconstriction could more easily evolve to irreversible lesions in the context of
ischemia-reperfusion inherent in the graft itself. At 1 year after transplantation the
reintroduction of CNIs at minimized doses could only moderately alter the renal function
allowing to maintain them at long term.
The purpose of this study is to demonstrate the feasibility of this transient treatment
strategy (from 3 to 12 months post transplantation) in patients with poor function at 3
months.
From 3 months post-transplantation, patients will receive for 9 months (phase 1) a treatment
with belatacept allowing to stop CNI. Then CNI will be reintroduced (phase 2) with a
follow-up period of 6 months which will make it possible to judge the feasibility of this
strategy.
Belatacept is the only biotherapy introduced successfully in transplantation. But this
treatment, because of the limitations raised, has not yet found a definite place. Our project
is to study a practical question: can the investigators stop belatacept after having
introduced it early in the context of an early dysfunction while preserving the benefits. The
decisive contribution of this study would be to prove the concept of a transient treatment by
belatacept which has not been reported. The medico-economic consequences would be major, the
cost of a long-term treatment by belatacept, especially because of its administration in
hospital, being much higher than that of a conventional treatment.
A secondary objective is to measure by flow cytometry the evolution of the absolute and
relative amount of regulatory T lymphocytes. Indeed, the negative effect of belatacept on
this essential lymphocyte population remains very controversial.
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