Nephrotic Syndrome Clinical Trial
Official title:
A Prospective, Sequential Study to Assess the Efficacy of Rituximab Therapy in Maintaining Remission of Nephrotic Syndrome After Steroid and Immunosuppressive Therapy Withdrawal in Patients With Steroid-dependant or Multirelapsing Minimal Change Disease or Focal Segmental Glomerulosclerosis (NEMO Study)
Background. Patients, especially children, with steroid-dependent or multirelapsing
nephrotic syndrome (NS) secondary to minimal change disease (MCD) or idiopathic focal and
segmental glomerulosclerosis (FSGS) on continuous treatment with steroids and/or other
immunosuppressive agents to limit or prevent recurrences are at increased risk of severe
drug-related adverse events. Case reports suggest that Rituximab, a B cell depleting
monoclonal antibody, could be a safe and effective alternative to steroid or
immunosuppressants to achieve and maintain remission in this population.
Objectives. The study is primarily aimed at evaluating whether Rituximab may maintain stable
NS remission after tapering and withdrawal of steroid and immunosuppressive therapy in
patients with MCD or FSGS and steroid-dependent or multirelapsing NS. Secondarily, the study
will assess whether Rituximab allows reducing maintenance doses of steroids and other
immunosuppressants (in those who relapse), thus limiting treatment related side effects and
costs.
Methods. This prospective, sequential, open, study will include 20 patients with histology
evidence of MCD or FSGS and steroid-dependant or multirelapsing NS, who are on stable
complete or partial remission since at least 1 month and, based on their previous history,
are expected to invariably relapse after steroid/immunosuppression withdrawal. After
baseline evaluation of clinical, laboratory and kidney function parameters [including
glomerular filtration rate (GFR), renal plasma flow (RPF), albumin and sodium fractional
clearance and the glomerular albumin permeability assay (Palb)], patients will receive one
Rituximab infusion that will be repeated 1 week later if CD20 cells are not fully depleted
from the circulation. Then ongoing immunosuppression will be progressively tapered up to
complete withdrawal over 6 to 9 months. 24h proteinuria will be monitored monthly and spot
urine will be tested daily by albustix to early detect disease relapses. Baseline
evaluations will be repeated at study end (1 year). Relapses will be treated with high-dose
steroids as per center practice and the last immunosuppressive therapy effective in
preventing disease reactivation will be reintroduced.
Expected results. Rituximab is expected to prevent NS recurrence following tapering and
discontinuation of steroid and other immunosuppressants. Maintaining remission without
chronic immunosuppression is expected to minimize risks and costs of therapy and to
remarkably improve patient outcomes.
BACKGROUND Nephrotic syndrome (NS)affects 2 every 100,000 children younger than 16 years.
Minimal change disease (MCD) accounts for around 90 percent of cases and most of the
remaining ones are associated with focal segmental glomerulosclerosis (FSGS). Patients with
NS are at increased risk for life-threatening infections and thromboembolic episodes, and
are often affected by dyslipidemia and osteoporosis. Glucocorticoids are first-line
treatment and may achieve remission in about 90% of patients with MCD and in 20 to 60% of
those with FSGS. In about 20% to 60% of those achieving remission, however, steroid
withdrawal is followed by a recurrence of the disease. These patients require chronic
steroid therapy (steroid-dependent cases): this prevents relapses in most cases but is
invariably associated with severe adverse effects including growth retardation, infections,
malignancies, hypertension, impaired glucose tolerance, weight gain and somatic changes. In
a small proportion of patients, recurrences occur even under chronic steroid therapy
(multirelapsing cases). In these cases, several approaches have been used to control disease
activity including plasmapheresis and add-on therapy with cyclophosphamide, cyclosporine,
mycophenolate mofetil and other immunosuppressants. Chronic immunosuppression, however,
seldom achieves persistent remission and is invariably burdened by serious adverse effects
including gonadotoxicity and sterility, opportunistic infections, malignancies, bone marrow
depression and renal toxicity. Thus, safer and more effective treatments are urgently needed
for these patients.
Rituximab, a chimeric monoclonal antibody targeted to the CD20 antigen of B cells able to
induce antibody-dependent and complement-mediated lysis of these cells, has been reported to
be effective in children with NS secondary to MCD or FSGS unresponsive to other
immunosuppressive treatments. Rituximab achieved persistent NS remission in a patient with
MCD diagnosed at age of 30 yrs who had a history of frequent relapses refractory to
treatment with other immunosuppressants. Thus, chronic MCD persisting into adult-years may
respond to rituximab and sustained remissions are possible despite long-term disease and
after other treatments have failed. Along the same line, rituximab achieved prompt and
persistent remission in an adult with steroid and mycophenolate mofetil-resistant MCD and in
two patients with FSGS and steroid-resistant NS.
The above findings suggest that rituximab may have a role in the treatment of patients who
require chronic exposure to steroids and/or other immunosuppressants to prevent or limit
disease reactivation. Thus, main goal of the present study is to assess whether rituximab
administration may allow tapering and withdrawing ongoing treatment without exposing the
patients to the risk of disease recurrence.
AIMS Primary
- To evaluate whether Rituximab therapy is able to prevent NS recurrence after complete
withdrawal of steroids and other immunosuppressive treatments in patients with
steroid-dependant or multirelapsing NS on sustained remission for at least 1 month.
Secondary
- To assess whether Rituximab therapy may reduce the need for steroids and other
immunosuppressive agents to prevent and treat further disease relapses;
- To evaluate whether tapering or withdrawal of immunosuppressant therapy is associated
with regression of the related toxicities, such as growth retardation, hypertension,
impaired glucose tolerance and dyslipidemia;
- To assess whether persistent NS remission is associated with an improvement of kidney
function and of renal hemodynamics;
- To study whether proteinuria remission is associated with the disappearance of albumin
permeability factor(s) from patient's sera;
- To assess the safety profile of the rituximab treatment;
- To evaluate the cost/effectiveness of the study treatment.
;
Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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