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Sponsored by: |
Lipomed |
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Information provided by: | Lipomed |
ClinicalTrials.gov Identifier: | NCT00349453 |
Systematical (retro- and prospective) investigation of the long-term safety (toxicity assessment according to CTCAE v3.0) and efficacy of deferiprone either given alone or in combination with desferrioxamine
Condition | Intervention | Phase |
---|---|---|
Hemochromatosis |
Drug: Deferiprone (L1) Drug: Desferrioxamine |
Phase II |
Study Type: | Interventional |
Study Design: | Treatment, Non-Randomized, Open Label, Uncontrolled, Parallel Assignment, Safety/Efficacy Study |
Official Title: | Retrospective and Prospective Multicenter Study Using Deferiprone (L1) Alone or in Combination With Desferrioxamine for the Treatment of Iron Overload in Transfusion-Dependent Patients |
Estimated Enrollment: | 30 |
Study Start Date: | March 2005 |
Patients with refractory anemias requiring regular blood transfusions accumulate iron at the rate of approximately 0.5 mg/kg/day, which may lead to serious organ toxicity, e.g. to the heart, liver and endocrine organs. The human body has no active mechanism for the excretion of excess iron. Therefore multiply transfused patients will develop a secondary hemosiderosis, if excess iron is not excreted by a chelating agent. Symptoms of iron-overload occur when body iron stores reach 10-20 g 2. At higher levels severe, even fatal complications, particularly cardiac failure, may develop.
Desferrioxamine (DFO, Desferal) is the established and commonly used iron-chelating drug, but is expensive and must be given by slow subcutaneous or intravenous infusion for 8-12 hours a day during 5-7 days weekly at a dosage of 40-50 mg/kg body weight/day. This often leads to failure of compliance of the patient and therefore to inefficient iron chelation. Further, some patients are hypersensitive to desferrioxamine and others suffer from toxicity, e.g. to the ears or eyes.
Deferiprone (L1; CP20; 1,2 dimethyl-3-hydroxypyrid-4-one) is an orally active iron chelator investigated in various clinical trials since 1987. Dosages of 75 - 100 mg/kg body weight/day of L1 have been considered effective to maintain stable iron balance (urinary iron excretion of 0.5 mg/kg/day) and to reduce serum ferritin levels between 6% and 25% within one year of treatment in iron-overloaded thalassemic patients. There exists long-term experience with patients who have received deferiprone continuously for more than 10 years so far. The main side effects encountered during a deferiprone therapy are arthropathy, gastrointestinal symptoms, headache, and mild zinc deficiency. These adverse reactions are usually reversed on reducing the dose or discontinuing the drug. Except for severe joint symptoms in few patients, most of the subjects in different clinical trials have been able to continue with L1 therapy for a long term. The most severe, but rare complication following administration of deferiprone is agranulocytosis or neutropenia.
A new treatment regimen combining deferiprone with desferrioxamine is currently being investigated in many countries. Preliminary data have demonstrated that the combined use of both drugs is highly active showing an additive or even synergistic effect (significant decrease of serum ferritin and hepatic iron content, increase of urinary iron excretion). This synergism could be explained by the different mode of action of the two drugs. It could be demonstrated that patients who were not sufficiently chelated with desferrioxamine or deferiprone, could achieve a negative iron balance with the combination treatment of both drugs. The combined regimen was generally well tolerated. It has been speculated that the individual toxicity profile of both drugs can be positively influenced by the simultaneous administration of L1 and DFO. The daily treatment with L1 tablets combined with at least twice a week administration of parenteral desferrioxamine is more patient-convenient and therefore may enhance the patient’s compliance.
The primary aim of this study is to systematically investigate the long-term safety (toxicity assessment according to CTCAE v3.0) of deferiprone either given alone or in combination with desferrioxamine. Further, in patients agreeing to perform annual SQUID analysis of the liver, the annual change of liver iron concentration (LIC) will be examined for four years.
Ages Eligible for Study: | 4 Years and older |
Genders Eligible for Study: | Both |
Accepts Healthy Volunteers: | No |
Inclusion Criteria:
Exclusion Criteria:
Contact: Claudia B von Orelli | 0041 61 715 96 82 | claudia.vonorelli@lipomed.com |
Switzerland | |
Private children clinic | Recruiting |
Bern, Switzerland, 3014 | |
Contact: Petrign FG Töndury, MD 0041 31 331 21 55 | |
Principal Investigator: Petrign FG Töndury, MD |
Principal Investigator: | Petrign FG Töndury, MD | Unaffiliated |
Principal Investigator: | Markus Schmugge Liner, MD | University Children's Hospital, Zurich |
Study ID Numbers: | DF-2/CH |
Study First Received: | July 6, 2006 |
Last Updated: | February 27, 2007 |
ClinicalTrials.gov Identifier: | NCT00349453 |
Health Authority: | Switzerland: Swissmedic |
Deferiprone L1 Desferrioxamine |
Hemochromatosis Iron overload Thalassemia |
Metabolism, Inborn Errors Metabolic Diseases Genetic Diseases, Inborn Deferiprone Hemochromatosis, type 3 Hemochromatosis |
Iron Metabolism Disorders Iron Overload Metabolic disorder Iron Thalassemia Deferoxamine |
Molecular Mechanisms of Pharmacological Action Iron Chelating Agents Chelating Agents |
Metal Metabolism, Inborn Errors Pharmacologic Actions Siderophores |