Chronic Renal Failure Clinical Trial
Official title:
The Effect of Steroid Pulse Therapy for the Reduction of Acute Rejection Episode in Subclinical Borderline Changes: An Open-Label, Randomized Clinical Trial
- Several studies have shown that about 30% of transplanted kidneys with stable function
present with tubule-interstitial mononuclear cell infiltration in protocol biopsies and
therefore meet criteria for acute rejection. This subclinical rejection (SCR) has also
been correlated with subsequent chronic allograft nephropathy and allograft
dysfunction.
- The Banff scheme defines the minimal threshold for acute T-cell mediated rejection as
infiltration of 25% or more of the renal cortex with five or more mononuclear cells in
a focus of tubulitis or intimal arteritis (histological indices i2t2 or v1) and refers
to borderline changes as those with insufficient for a diagnosis of acute T-cell
mediated rejection, including mild to moderate (<50%) cortical infiltration and one to
four mononuclear cells per tubule in cross section (i1t1 or i2t1)
- No consensus for the treating patients with borderline changes has been reached.
Borderline changes with graft dysfunction are occasionally routinely treated with
steroid pulse and, whereas subclinical borderline changes are simply 'ignored'.
Particularly, a previous study demonstrated that most cases designated borderline by
histopathology are found to be non-rejection by molecular phenotyping
- The aim of this study is to investigate the effect of early steroid pulse therapy for
the reduction of acute rejection episode during the first year after renal
transplantation in the patients who will show subclinical borderline changes at 2-week
protocol biopsy.
Background
Several studies have shown that about 30% of transplanted kidneys with stable function
present with tubule-interstitial mononuclear cell infiltration in protocol biopsies and
therefore meet criteria for acute rejection (1). This subclinical rejection (SCR) has also
been correlated with subsequent chronic allograft nephropathy and allograft dysfunction
(2,3).
The Banff 97 working classification of renal allograft pathology was introduced to
standardize the histological definition of acute allograft rejection and to guide treatment
of renal transplant recipients (4,5). The Banff scheme defines the minimal threshold for
acute T-cell mediated rejection as infiltration of 25% or more of the renal cortex with five
or more mononuclear cells in a focus of tubulitis or intimal arteritis (histological indices
i2t2 or v1) and refers to borderline changes as those with insufficient for a diagnosis of
acute T-cell mediated rejection, including mild to moderate (<50%) cortical infiltration and
one to four mononuclear cells per tubule in cross section (i1t1 or i2t1) (6).
The averaged prevalence of borderline SCR at 1-2 week is 24% (range 12-38%), at 1-2 months
is 23% (range 21-27%), at 2-3 months is 23% (range 11-41%) and 1 year is 17% (range 7-44%)
from selected studies (7). However, the pathogenic role of such limited cortical mononuclear
infiltration is not well established and no consensus for the treating patients with
borderline changes has been reached. In practice, borderline changes with graft dysfunction
are occasionally routinely treated with steroid pulse and, whereas subclinical borderline
changes are simply 'ignored'. Particularly, a previous study demonstrated that most cases
designated borderline by histopathology are found to be non-rejection by molecular
phenotyping (8). Furthermore, some previous studies have shown that the risk of infection is
higher in patients receiving high dose steroid (9-12), and a previous study suggested that
the infection risk was increased, up to as 1.5-fold, in patients receiving steroid pulse
therapy (SPT) for acute rejection (13).
Some previous studies revealed that the graft survival rates with treated borderline SCR was
99.1% at 1-year, 95.1% at 5-years, and 93.7% at 10-years (14) and the graft survival rates
with untreated borderline SCR was 90.9% at 1-year (15). However, there was no randomized
controlled study on the effect of steroid pulse therapy in stable renal transplant
recipients with subclinical borderline changes.
Purpose
- The reduction in risk of graft failure is the pivotal measure of effectiveness for
evaluating immunosuppressive regimens for renal transplantation. However, because of
the long follow-up periods and large sample size required for such an endpoint,
randomized controlled trials of immunosuppressive therapies have mostly relied on the
surrogate endpoints.
- In our institution, since routine protocol biopsies are performed at 2 weeks, 1 year,
and 2 years after renal transplantation, it is practically difficult that graft
survival is used as an endpoint for randomized controlled trials.
- From a meta-analysis for 31 observational studies (16), acute rejection was associated
with an increased risk of graft loss risk ratios ranged from 1.2 - 10.5. Furthermore,
chronic allograft nephropathy and graft survival is strongly correlated with acute
rejection episode during the first year after renal transplantation (17,18).
- Therefore, the aim of this study is to investigate the effect of early steroid pulse
therapy for the reduction of acute rejection episode during the first year after renal
transplantation in the patients who will show subclinical borderline changes at 2-week
protocol biopsy.
- To evaluate the benefit over the risk, this study also investigates the effect of early
steroid pulse therapy on the opportunistic infection including bacterial, fungal, and
viral infections.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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