Microscopic Polyangiitis Clinical Trial
Official title:
A Pilot Study of Mycophenolate Mofetil (MMF) in Patients With p-ANCA Microscopic Polyangiitis and Mild to Moderate Renal Dysfunction.
Microscopic polyangiitis (MP) is a primary systemic vasculitis predominantly affecting small blood vessels. Following the widespread introduction of ANCA testing, the primary systemic vasculitis (SV), Wegener?s granulomatosis (WG) and microscopic polyangiitis (MP) appear to be more frequent than was previously thought (see definitions in Appendix 6). In addition, the existence of early and organ-limited forms of these diseases, such as renal-limited vasculitis (RLV) is now clearly recognized. Their annual incidence exceeds 20 per million per year and they account for at least 5 % of the causes of end stage renal failure. The two diseases share many features of their histology, serology and response to treatment, pointing to similarities in their pathogenesis, which have justified a common approach to their management. The standard treatment with corticosteroids (CS) and cyclophosphamide (CYC) is usually effective at controlling active disease but continued treatment is necessary to prevent disease relapse. Due to the cumulative toxicity associated with CYC treatment, alternatives have been looked for. Mycophenolate mofetil (MMF) has been used to treat patients with a variety of immune-mediated nephritides, including ANCA-associated vasculitis, with less toxicity than CYC but with variable outcome. The present trial will examine whether substitution of oral CYC with oral MMF is equally efficient for induction of remission with less adverse effects in cases of MP with mild to moderate renal involvement. All patients will receive the same regimen of oral prednisone + MMF. Prednisone will be tapered to a stop after 24 weeks but MMF will continue for a total of 18 months unless there is worsening or persistent disease. The trial ends after 18 months.
1. Patients will receive I.V. methylprednisone, or I.V. dexamethazone, oral prednisone and
oral MMF therapy as outlined in table 2.
2. MMF will be initiated within the first 1-2 weeks of the start of steroids. Patients
will receive CellCept, 750 mg po b.i.d for the first week. Dose will be increased to
1000 mg po b.i.d for the second week, and thereafter, according to blood levels and
patient tolerance. Target blood levels are 1 ? 3.5 g/ml. Treatment will be for
a total of 18 months. This is based on the published dose-dependent adverse effect
profiles in transplant patients (31-32) and on reports that lower doses are ineffective
and shorter courses (less then 6 months) result in relapses or failure of therapy (25).
Dose will be reduced in patient who can not tolerate MMF at the above dose.
2) Relapse treatment to follow guidelines for relapse regimens. 3) After 18 months, all
medications will be tapered to a full stop unless disease is active or grumbling.
4) Pneumocystis pneumonia prophylaxis will be used during the trial (with
sulfamethoxazole/trimethoprim, or Dapsone or Mepron if allergic to sulfa).
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Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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