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Clinical Trial Summary

Patients with thalassemia intermedia, congenital dyserythropoietic anemia type I , and sideroblastic anemia were found to express very high levels of serum GDF15, and this contributed to the inappropriate suppression of hepcidin with subsequent secondary iron overload.The aim of our present study is to asses the levels of GDF15 and hepcidin in patients with Sickle cell disease and hereditary spherocytosis


Clinical Trial Description

The identification of the ferroportin/hepcidin axis has allowed the effect of erythroid activity on iron balance to be studied and has created the basis for better defining the erythroid regulators.

In iron-loading anemias, ineffective erythropoiesis suppresses hepcidin production, which result in dysregulating iron homeostasis. Miller and co-workers showed that release of cytokines like growth differentiation factor 15 (GDF15) during the process of ineffective erythropoiesis inhibits hepcidin production, thus defining a molecular link between ineffective erythropoiesis, suppression of hepcidin production and parenchymal iron loading. ;


Study Design

Time Perspective: Prospective


Related Conditions & MeSH terms


NCT number NCT01201135
Study type Observational
Source Wolfson Medical Center
Contact Ghoti Hossam, doctor
Phone 035028110
Email drghoti123@yahoo.com
Status Not yet recruiting
Phase N/A
Start date September 2010
Completion date September 2011