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CellCept/Iron Study: The Iron Ion-Mycophenolate Mofetil Chelation Complex Interaction in Renal Allograft Recipients

Sponsor
University of Michigan (Other)
Overall Status
Completed
CT.gov ID
NCT00227045
Collaborator
Hoffmann-La Roche (Industry)
20
Enrollment
1
Location

Study Details

Study Description

Brief Summary

The objective of this study is to determine the extent and magnitude of the pharmacokinetic drug interaction between mycophenolate mofetil (MFF) (under Css conditions) in the presence of iron in renal transplant recipients.

A two phase pharmacokinetic study will be conducted to determine the bioavailability of MMF (under steady state, Css, conditions) in the presence of two commonly prescribed iron formulations (polysaccharide iron complex and sustained release ferrous sulfate) in renal transplant recipients. This study will evaluate valuable clinical information to help better guide the appropriate utilization of the following formulations and dosing strategies:

  1. Polysaccharide iron complex concomitant administration with MMF,

  2. Sustained release ferrous sulfate concomitant administration with MMF,

  3. Dose separation (2 hours) between MMF and iron (polysaccharide iron complex or sustained release [S.R.] ferrous sulfate)

Condition or Disease Intervention/Treatment Phase

    Detailed Description

    Following oral administration, MMF is rapidly absorbed and is presystemically hydrolyzed to its active form MPA in the liver. It is then metabolized by glucuronyl transferase to its inactive metabolite mycophenolic acid glucuronide (MPAG). MPA and MPAG also undergo a significant enterohepatic recirculation process, which is thought to contribute to the secondary peaks in the serum concentrations.

    Pharmacokinetic studies in healthy volunteers have demonstrated the bioavailability to be ~94%. Previous studies have shown that many concomitantly administered medications including magnesium and aluminum containing antacids and cholestyramine, significantly impair bioavailability and decrease serum MPA AUCs from 37% and 40%, respectively.

    However, of the potentially significant drug interactions involving MMF, iron may have the most clinically significant consequences. A large portion of the transplant population, particularly renal allograft recipients, experience anemia requiring iron supplementation. A single dose pharmacokinetic study conducted in seven healthy volunteers evaluated the effect of concomitant iron (delayed release preparation) administration on the absorption of MMF. This study reported a significant (89.7%) decrease in AUC among patients receiving concomitant iron and MMF. Although this study provides valuable information, it fails to address several clinically pertinent questions for transplant clinicians including:

    1. the potential impact on steady state MPA kinetics in transplant patients,

    2. effect of immediate release iron preparation compared with sustained release iron product, and

    3. the effect of timing of the dose relative to administration of MMF.

    Study Design

    Study Type:
    Observational
    Observational Model:
    Defined Population
    Time Perspective:
    Other
    Official Title:
    The Iron Ion-Mycophenolate Mofetil Chelation Complex Interaction: A Two Phase Pharmacokinetic Study in Renal Allograft Recipients at the University of Michigan Transplant Program
    Study Start Date :
    Oct 1, 2003

    Outcome Measures

    Primary Outcome Measures

      Eligibility Criteria

      Criteria

      Ages Eligible for Study:
      18 Years and Older
      Sexes Eligible for Study:
      All
      Accepts Healthy Volunteers:
      No
      Inclusion Criteria:

      • Patients prescribed iron and mycophenolate mofetil concomitantly

      • The subject must be able to give informed consent for the study.

      • Stable renal transplant patients age 18 years and older.

      • At least 6 months status-post primary or secondary kidney transplant.

      • Stable organ function

      • Patients who have achieved therapeutic levels of cyclosporine, tacrolimus, or sirolimus.

      • Patients on stable doses of cyclosporine, tacrolimus, or sirolimus. Defined as: No dosage adjustments within 2 weeks prior to study entry.

      • Patients receiving ferrous sulfate iron preparations (either sustained release or immediate release preparations) or polysaccharide iron complex

      Exclusion Criteria:

      • Treated for acute rejection within the last 90 days

      • Received other organ transplants in addition to kidney

      • Pregnant or breast-feeding

      • Use of iron supplements other than ferrous sulfate or polysaccharide iron complex

      Contacts and Locations

      Locations

      Site City State Country Postal Code
      1 University of Michigan Ann Arbor Michigan United States 48109

      Sponsors and Collaborators

      • University of Michigan
      • Hoffmann-La Roche

      Investigators

      • Principal Investigator: Jeong Park, PharmD, University of Michigan Hospital

      Study Documents (Full-Text)

      None provided.

      More Information

      Publications

      None provided.
      Responsible Party:
      , ,
      ClinicalTrials.gov Identifier:
      NCT00227045
      Other Study ID Numbers:
      • CEL305
      First Posted:
      Sep 27, 2005
      Last Update Posted:
      Apr 20, 2007
      Last Verified:
      Apr 1, 2007
      Keywords provided by , ,
      Kidney Transplantation
      Additional relevant MeSH terms:
      Kidney Failure, Chronic

      Study Results

      No Results Posted as of Apr 20, 2007