Diabetes Mellitus Clinical Trial
Official title:
Treatment of Wolfram Syndrome Type 2 With the Chelator Deferiprone, and Incretin Based Therapy
Patients who are genetically diagnosed with the recently reported and rare Wolfram syndrome type 2 ( WFS2) and have the degenerative and symptomatic disease including signs such as diabetes, platelet aggregation defect or visual problems will be asked to participate in this study. Knowing the pathomechanism of WFS2 with rapid cell death, after doing baseline investigations to asses the severity of their disease, the participants will be offered a chelator therapy with in addition to the antioxidant Acetylcystein, in diabetic patients an Incertin (GLP-1 ) therapy will be offered as well. The baseline investigations will be repeated after 2 months and after 5 months of therapy in order to asses the progression of the disease and to show if the chelator and anti oxidant therapy and in diabetic patients the GLP-1 therapy could stop the progression of the disease.
In WFS2 mutation the protein nutrient-deprivation autophagy factor-1(NAF-1) is affected.
Given the known result of NAF-1 protein dysfunction in animal and cultured cell line models
namely a toxic accumulation of iron in the mitochondria,leading to mitochondrial destruction
and oxidative stress we aim to obtain fibroblast samples from the patients and (use
laboratory fibroblasts from healthy subjects as controls) These cell cultures will initially
be studied for intracellular iron accumulation and then re-evaluated following treatment by
Deferiprone and/or Glucagon-like peptide 1 (GLP-1) ex-vivo in the laboratory .
If repeated (n>=3) histological evidence confirms the beneficial effect of Deferiprone
and/or GLP-1(incertin based therapy) in the patient's cultured fibroblasts by reversing the
toxic iron accumulation in the patient's mitochondria to a normal level, he/she will be
offered "in vivo" therapy using the oral chelating agent - with or without
dipeptidylpeptidase-4 inhibitor (DPP-4) inhibitors or GLP-1 receptor agonists. Adding GLP-1
based therapy will depend on the diabetic status of the patient.
Prior and following 60 and 150 days of Chelator and/or GLP-1 therapy they will go through
the following clinical and laboratory evaluations which will establish the baseline and post
therapeutic parameters (outcome) to be compared:
detailed medical history and physical examination complete blood count (CBC) and iron levels
platelet aggregation studies Fundoscopy and visual evoked potentials (VEP) Hearing
evaluation Oral glucose Tolerance Test optional Intra venous glucose tolerance test (IVGTT)
/glucagon/arginine test HBA1C Daily profile of blood glucose Optional CGMS ( continuous
glucose monitoring system) Gastroscopy and gastric biopsy if the patient suffers from
abdominal pain, hematemesis, melena or iron deficiency anemia or if peptic ulcer disease is
clinically suspected.
Based on the routine use of the iron chelator, FDA approved, Deferiprone for Thalassemia
(with detailed official guidelines of the Israel association for Pediatric Hematology) and
for a similar subcellular iron accumulating disease - e.g. Friedreich Ataxia, we will
initially use a dose of 20 mg per kilogram body weight (BW) daily divided in two equal
doses. N-Acetylcystein an over the counter drug which also is an anti-oxidant will be given
orally in the dose of 200mg twice daily to have a synergistic effect with Deferiprone.
In addition if they suffer from diabetes they will receive Januet (Sitagliptin/metformin) .
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Allocation: Non-Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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