Atypical Hemolytic Uremic Syndrome Clinical Trial
— aHUSOfficial title:
An Open-label, Multi-center Controlled Clinical Trial of Eculizumab in Adult Patients With Plasma Therapy-sensitive Atypical Hemolytic Uremic Syndrome (AHUS)
The purpose of this study is to determine whether eculizumab is safe and effective in the treatment of adult patients with plasma therapy-sensitive Atypical Hemolytic-Uremic Syndrome (aHUS).
Status | Completed |
Enrollment | 15 |
Est. completion date | December 2013 |
Est. primary completion date | October 2010 |
Accepts healthy volunteers | No |
Gender | Both |
Age group | 18 Years and older |
Eligibility |
Inclusion Critera: 1. Male or female patients' =18 years of age who have been diagnosed with Atypical Hemolytic-Uremic Syndrome (aHUS). 2. Patients must be receiving PT for aHUS and must be observed to receive = 1 PT treatment every two weeks and no more than 3 PT treatments/week (at an unchanged frequency) for at least 8 weeks before first dose of IP. 3. Platelet Count Pre-PT Baseline Set-Point (collected in the hours before the Qualifying PT Episode) is within 75% of the average of the Pre-PT platelet counts collected at Screening and during the Observation Period. 4. Known complement regulatory protein genetic abnormality. 5. Lactate dehydrogenase (LDH) level at screening or at the onset of the current aHUS episode was = ULN. If LDH is normal at screening, other markers indicative of ongoing hemolysis such as haptoglobin, schistocytes should be evaluated and discussed with Sponsor. 6. Creatinine level = ULN for age. 7. Female patients of childbearing potential must be practicing an effective, reliable and medically approved contraceptive regimen during the entire duration of the study, including the follow-up period and for up to 5 months following eculizumab treatment discontinuation. 8. Able to give written informed consent. 9. Able and willing to comply with study procedures. Exclusion Criteria: 1. TTP, (defined as ADAMTS-13 activity <5%) from an historical observation (prior to initiation of plasma therapy) or as tested at the screening visit by the central laboratory. 2. Malignancy within 5 years of screening. 3. Typical HUS (Shiga toxin +). 4. Known HIV infection. 5. Identified drug exposure-related HUS. 6. Infection-related HUS. 7. HUS related to bone marrow transplant. 8. HUS related to vitamin B12 deficiency. 9. Patients with a confirmed diagnosis of sepsis. 10. Presence or suspicion of active and untreated systemic bacterial infection that, in the opinion of the Investigator confounds an accurate diagnosis of aHUS or impedes the ability to manage the aHUS disease. 11. Pregnancy or lactation. 12. Unresolved meningococcal disease. 13. Known Systemic Lupus Erythematosus (SLE) or antiphospholipid antibody positivity or syndrome. 14. Any medical or psychological condition that, in the opinion of the investigator, could increase the patient's risk by participating in the study or confound the outcome of the study. 15. Patients who have received previous treatment with eculizumab. 16. Patients receiving IVIg within 8 weeks or Rituximab therapy within 12 weeks of the screening visit. 17. Patients receiving other immunosuppressive therapies such as steroids, mTOR inhibitors or tacrolimus are excluded unless: [1] part of an established post-transplant anti-rejection regime, [2] patient has confirmed anti-CFH antibody requiring immunosuppressive therapy, and [3] dose of such medications have been unchanged for at least 4 weeks prior to the screening period and throughout the Observation Period or [4] patient is experiencing an acute aHUS relapse immediately after transplant. 18. Patients receiving Erythrocyte Stimulating Agents (ESAs) unless already on a stable dose for at least 4 weeks prior to the screening period, or a washout period of at least 2 weeks from the last dose of ESA therapy. 19. Participation in any other investigational drug trial or exposure to other investigational agent, device, or procedures beginning 4 weeks prior to screening and throughout the entire trial. 20. Hypersensitivity to eculizumab, to murine proteins or to one of the excipients. |
Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
Country | Name | City | State |
---|---|---|---|
n/a |
Lead Sponsor | Collaborator |
---|---|
Alexion Pharmaceuticals |
Canada, France, Germany, Italy, Netherlands, Sweden, United Kingdom,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Percentage of Patients With TMA Event-free Status | TMA Event-free status is defined as the absence for at least 12 weeks of [1] decrease in platelet count of > 25% from the Platelet Count Pre-PT Baseline Set Point; [2] PT while the patient is receiving eculizumab, and [3] new dialysis. | Through 26 weeks | No |
Primary | Percentage of Patients With Hematologic Normalization | Hematologic Normalization was defined as normalization of both platelet count and lactic dehydrogenase (LDH) sustained for at least two consecutive measurements which spanned a period of at least four weeks. | Through 26 weeks | No |
Primary | Percentage of Patients With Complete TMA Response | The proportion of patients who achieved a Complete TMA Response from baseline through 26 weeks of treatment with eculizumab was determined. Complete TMA Response was defined as Hematologic Normalization plus improvement in renal function (defined as (=25% reduction from baseline in serum creatinine), which was sustained for two consecutive measurements over a period of at least four weeks. | Through 26 weeks | No |
Secondary | TMA Intervention Rate | TMA Intervention Rate (# PE/PI and # Dialysis Events/Patient/Day) in the eculizumab treatment period (from baseline through 26 weeks) for PE/PI and (from the fifteenth day following the first eculizumab dose through 26 weeks) for new dialysis events was compared with the TMA Intervention Rate during the pre-eculizumab treatment period. | Through 26 weeks | No |
Secondary | Platelet Count Change From Baseline to 26 Weeks | From Baseline to 26 Weeks | No | |
Secondary | Percentage of Patients With Platelet Count Normalization | Platelet count normalization was defined as the platelet count observed to be =150 x 10^9/L on at least two consecutive measurements which span a period of at least four weeks | Through 26 Weeks | No |
Secondary | Percentage of Patients With TMA Event-free Status | TMA Event-free status is defined as the absence for at least 12 weeks of [1] decrease in platelet count of > 25% from the Platelet Count Pre-PT Baseline Set Point; [2] PT while the patient is receiving eculizumab, and [3] new dialysis. | Through End of Study, Median Exposure 156 Weeks | No |
Secondary | Percentage of Patients With Hematologic Normalization | Hematologic Normalization was defined as normalization of both platelet count and lactic dehydrogenase (LDH) sustained for at least two consecutive measurements which spanned a period of at least four weeks. | Through End of Study, Median Exposure 156 Weeks | No |
Secondary | Percentage of Patients With Complete TMA Response | The proportion of patients who achieved a Complete TMA Response from baseline through end of study with eculizumab was determined. Complete TMA Response was defined as Hematologic Normalization plus improvement in renal function (defined as (=25% reduction from baseline in serum creatinine), which was sustained for two consecutive measurements over a period of at least four weeks. | Through End of Study, Median Exposure 156 Weeks | No |
Secondary | TMA Intervention Rate | TMA Intervention Rate (# PE/PI and # Dialysis Events/Patient/Day) in the eculizumab treatment period (from baseline through end of study) for PE/PI and (from the fifteenth day following the first eculizumab dose through end of study) for new dialysis events was compared with the TMA Intervention Rate during the pre-eculizumab treatment period. | Through End of Study, Median Exposure 156 Weeks | No |
Secondary | Platelet Count Change From Baseline to 156 Weeks | From Baseline to 156 Weeks | No | |
Secondary | Percentage of Patients With Platelet Count Normalization | Platelet count normalization was defined as the platelet count observed to be =150 x 10^9/L on at least two consecutive measurements which span a period of at least four weeks Not specified. | Through End of Study, Median Exposure 156 Weeks | No |
Secondary | Pharmacokinetics (PK) and Pharmacodynamics (PD); Minimum and Maximum Blood Concentration | Induction Phase for 4 weeks followed by Maintenance Phase starting on Week 5 through 26 weeks or longer. | No |
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