Hemochromatosis Clinical Trial
Official title:
Therapeutic Effect of Erythrocyte Apheresis as Compared to Full Blood Phlebotomy in Patients With Hereditary Hemochromatosis
Primary hemochromatosis is the most frequent hereditary condition in Scandinavia. The
condition may result in serious organ damage which can be prevented by therapy, but only few
patients develop such organ damage. The optimal treatment, therefore, is still a matter of
discussion Prevention of organ damage has traditionally been accomplished by drawing of full
blood (phlebotomy), which has to be frequently repeated during the initial phase and then
continued indefinitely as a maintenance treatment. The removed amount of iron may be
increased two- or threefold for each procedure by using modern equipment for selective
removal of red blood cells (red cell apheresis). Possible drawbacks of this technique may be
higher costs, prolonged time for each therapeutic procedure, and certain requirements to the
patients. The possible advantages are the reduced number of therapeutic procedures and less
strain for the patient. No larger, randomized study has been published in order to determine
which method should be preferred.
This study is a controlled trial in which participating patients are asked to be randomized
to red cell apheresis or traditional phlebotomy. Each group will be followed by means of
well-defined assessments in order to explore possible advantages and disadvantages of each
method in order to establish what type of treatment should be recommended.
Introduction Primary hemochromatosis is the most frequent hereditary condition in
Scandinavia. The condition may result in serious organ damage which can be prevented by
therapy, but only few patients develop such organ damage. Provided the lack of more exact
knowledge of which patients should be treated, we have based our inclusion criteria on the
guidelines published by the Norwegian Society of Hematology. However, the criteria for
ferritin levels have been set at 300 micrograms/L for patients who are homozygous for the
C282Y mutation, and also heterozygous individuals will be included if ferritin is higher
than 500 micrograms/L.
Furthermore, the optimal treatment method is still a matter of discussion. Prevention of
organ damage has traditionally been accomplished by whole blood phlebotomy, which has to be
frequently repeated during the initial phase and then continued indefinitely as a
maintenance treatment. The removed amount of iron may be increased two- or threefold for
each procedure by using modern equipment for selective withdrawal of red blood cells
(erythrocyte apheresis). Possible drawbacks of this technique may be higher costs, prolonged
time for each therapeutic procedure, and certain requirements to the patients. The possible
advantages are the reduced number of therapeutic procedures and less strain for the patient.
No larger, randomized study has been published in order to determine which method should be
preferred.
Hypothesis: A more rapid decline of primary endpoints (see below) can be achieved by
erythrocyte apheresis as compared to traditional phlebotomy, without significant
disadvantages.
Design The trial is prospective, randomized and open. Eligible patients are randomized to
erythrocyte apheresis and phlebotomy.
Endpoints Primary endpoints Decline of ferritin levels and transferrin saturation.
Secondary endpoints and other variables to be studied Decline in hemoglobin levels.
Discomfort during the therapeutic procedure. Any changes in EVF, blood cell counts or
albumin and CRP levels. Certain well-defined financial costs: consumed material, technician
working time.
Inclusion criteria
1. Diagnosis
1. Individuals who art homozygous for C282Y or H63D or "compound heterozygous" for
these tow variants and have ferritin levels higher than 300 micrograms/L or
transferrin saturation higher than 50%.
2. Individuals heterozygous for C282Y or H63D if ferritin levels higher than 500
micrograms/L or transferrin saturation higher than 50%.
2. Requirements to the patient Body weight higher than 65 kg and initial hemoglobin level
higher than 12 g/dL.
Treatment schedule Following randomization to either apheresis or phlebotomy, patients are
treated until ferritin levels have declined to below 50 micrograms/L and they are then
followed for one year. Patients randomized to apheresis are treated every second week,
whereas patients in the phlebotomy group are treated weekly. Prolongation of the interval is
permitted in both groups in case of well-defined clinical indications. Any prolongation is
to be recorded along with the clinical indication.
Follow-up Clinical symptoms, body weight, laboratory findings (Hemoglobin levels; blood cell
counts; levels of iron, transferrin, ferritin, albumin and IgG; serologic assessments for
hepatitis viruses, CMV and HIV), discomfort during the therapeutic procedure, duration of
each procedure, costs for consumed material, working time of the technician for each
procedure.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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