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Pomalidomide and lenalidomide regulate erythropoiesis and fetal hemoglobin production in human CD34+ cells

机译:泊马度胺和来那度胺调节人CD34 +细胞中的红细胞生成和胎儿血红蛋白生成

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摘要

Sickle-cell disease (SCD) and β thalassemia constitute worldwide public health problems. New therapies, including hydroxyurea, have attempted to augment the synthesis of fetal hemoglobin (HbF) and improve current treatment. Lenalidomide and pomalidomide are members of a class of immunomodulators used as anticancer agents. Because clinical trials have demonstrated that lenalidomide reduces or eliminates the need for transfusions in some patients with disrupted blood cell production, we investigated the effects of lenalidomide and pomalidomide on erythropoiesis and hemoglobin synthesis. We used an in vitro erythropoiesis model derived from human CD34+ progenitor cells from normal and SCD donors. We found that both compounds slowed erythroid maturation, increased proliferation of immature erythroid cells, and regulated hemoglobin transcription, resulting in potent induction of HbF without the cytotoxicity associated with other HbF inducers. When combined with hydroxyurea, pomalidomide and, to a lesser extent, lenalidomide were found to have synergistic effects on HbF upregulation. Our results elucidate what we believe to be a new mechanism of action of pomalidomide and lenalidomide and support the hypothesis that pomalidomide, used alone or in combination with hydroxyurea, may improve erythropoiesis and increase the ratio of fetal to adult hemoglobin. These findings support the evaluation of pomalidomide as an innovative new therapy for β-hemoglobinopathies.
机译:镰状细胞病(SCD)和β地中海贫血构成全球范围内的公共卫生问题。包括羟基脲在内的新疗法已尝试增加胎儿血红蛋白(HbF)的合成并改善目前的治疗方法。来那度胺和泊马利度胺是用作抗癌剂的一类免疫调节剂的成员。由于临床试验表明来那度胺减少或消除了某些血细胞生成受阻患者的输血需求,因此我们研究了来那度胺和波马来度胺对红细胞生成和血红蛋白合成的影响。我们使用了来自正常和SCD供体的人CD34 + 祖细胞的体外红细胞生成模型。我们发现这两种化合物减慢了类红细胞的成熟,增加了未成熟的类红细胞的增殖,并调节了血红蛋白的转录,从而有效诱导了HbF,而没有与其他HbF诱导剂相关的细胞毒性。当与羟基脲结合使用时,波马来胺和来那度胺对HbF上调具有协同作用。我们的结果阐明了我们认为是泊马利度胺和来那度胺的新作用机理,并支持了泊马利度胺单独或与羟基脲联合使用可改善红细胞生成和增加胎儿与成人血红蛋白比例的假设。这些发现支持将泊马度胺作为一种创新的β-血红蛋白病新疗法的评估。

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