Nephrosis Clinical Trial
Official title:
Pulse Dexamethasone Over 48 Weeks for Podocyte Disease
Focal segmental glomerulosclerosis (FSGS) and minimal change disease are kidney diseases
that are associated with increased excretion of protein in the urine. Approximately half of
FSGS patients will lose kidney function within 8 years of diagnosis and will require
dialysis. The purpose of this study is to determine whether intermittent oral steroid
therapy can cause sustained remission of FSGS and MCD.
Approximately 70 participants, including adults and children older than age 2, will be
enrolled in this study. They will receive 48 doses of oral dexamethasone over a period of 48
weeks. One group will take two daily doses every 2 weeks; the other group will take four
daily doses every 4 weeks. Doctors will monitor participants before, during, and after the
steroid treatment with extensive exams and testing. At the completion of the study,
researchers will evaluate the safety and efficacy of the drug treatment.
The major causes of primary nephritic syndrome in adults and children are idiopathic
podocyte diseases, minimal change (MCD) and focal segmental glomerulosclerosis (FSGS). Our
objective is to determine whether intermittent oral dexamethasone administered over 48 weeks
can induce complete remission in these patients. This is an open-label multi-center pilot
study designed to obtain preliminary evidence of efficacy and to establish safety. This is
part of a long-term effort to define the most effective mode of administering pulse
dexamethasone and is expected to lead to a trial comparing daily prednisone to pulse
dexamethasone.
We will enroll up to 70 patients with nephritic-level proteinuria due to biopsy-proven MCD
(up to 30 patients) or FSGS (up to 40 patients). We will include adults and children greater
than 2.0 years of age. Children with MCD must have received a minimum of 4 weeks and a
maximum of 10 weeks of high-dose daily steroids, since many children are responsive to short
courses of daily steroids; these requirements will define a steroid-resistant population.
For children with FSGS and adults with MCD or FSGS, there is no minimum duration of prior
steroids and there is a maximum of 8 weeks of prior high-dose daily steroids; these
requirements will define a population that has received a short steroid course without
response. If steroids have been used, inclusion criteria require persistent nephrotic
syndrome (thus excluding steroid-sensitive nephrotic syndrome, whether steroid-dependent or
frequently relapsing).
Patients may enroll at NIH or at collaborating centers. Those patients who enroll at NIH
will visit the NIH Clinical Center at least 4 times. Patients enrolled at collaborating
centers have the option to come to the NIH Clinical Center to complete research tests; under
these circumstances they will be enrolled as NIH research subjects.
Patients will receive 48 doses of oral dexamethasone over a period of 48 weeks. Patients
will be randomized to one of two arms: 2 daily doses every 2 weeks or 4 daily doses every 4
weeks. The rationale is to test whether increased frequency dosing has greater efficacy with
acceptable safety. For adult patients, we have a record of safety with pulse dexamethasone
from the FSGS Dexamethasone study as well as from published studies for other diseases.
Therefore, for adults each pulse will be 50 mg/m(2) during the first 12 weeks and each pulse
will be 25 mg/m(2) during the next 36 weeks. The trial for pediatric patients involves dose
escalation, as there is little experience with pulse dexamethasone for podocyte diseases in
this age group. In pediatric stage 1, each dexamethasone pulse will be 25 mg/m(2) over 48
weeks. When 4 patients in each arm have completed 48 weeks of therapy, safety and efficacy
will be evaluated. If the evaluation is positive, we will embark on pediatric stage 2, in
which dexamethasone pulses will be 50 mg/m(2) during the first 12 weeks and 25 mg/m(2)
during the next 36 weeks (the same as the adult regimen).
The primary endpoint will be the presence of complete remission 48 weeks after beginning
therapy. Secondary endpoints will include complete and partial remission at 48 weeks, and
complete and partial remission at 104 weeks. Assessment of remission will be by 24 hour
urine collection in adults and children greater than 13.0 years and first void urine samples
in children less than 13.0 years. Patients will be evaluated for manifestations of steroid
toxicity, including growth rate (children), ophthalmologic complications, adrenal
suppression, osteoporosis, a vascular necrosis, and psychological disturbances.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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