In human
beta-thalassemia, the imbalance between alpha- and non-
alpha-globin chains causes ineffective erythropoiesis,
hemolysis, and
anemia: this condition is effectively treated by an enhanced level of
fetal hemoglobin (HbF). In spite of extensive studies on pharmacologic induction of HbF synthesis, clinical trials based on HbF reactivation in
beta-thalassemia produced inconsistent results. Here, we investigated the in vitro response of beta-thalassemic erythroid progenitors to
kit ligand (KL) in terms of HbF reactivation, stimulation of effective erythropoiesis, and inhibition of apoptosis. In unilineage erythroid cultures of 20 patients with intermedia or major
beta-thalassemia, addition of KL, alone or combined with
dexamethasone (Dex), remarkably stimulated cell proliferation (3-4 logs more than control cultures), while decreasing the percentage of apoptotic and dyserythropoietic cells (<5%). More important, in both thalassemic groups, addition of KL or KL plus Dex induced a marked increase of
gamma-globin synthesis, thus reaching HbF levels 3-fold higher than in con-trol cultures (eg, from 27% to 75% or 81%, respectively, in
beta-thalassemia major). These studies indicate that in
beta-thalassemia, KL, alone or combined with Dex, induces an expansion of effective erythropoiesis and the reactivation of
gamma-globin genes up to fetal levels and may hence be considered as a potential therapeutic agent for this disease.