羟基脲治疗需要诱导胎儿血红蛋白(HbF)产生才能对镰状细胞小鼠模型产生临床获益。
Hydroxyurea therapy requires HbF induction for clinical benefit in a sickle cell mouse model.
机构信息
Department of Hematology, St. Jude Children's Research Hospital, Memphis, TN 38105, USA.
出版信息
Haematologica. 2010 Sep;95(9):1599-603. doi: 10.3324/haematol.2010.023325. Epub 2010 Apr 7.
Abstract
Hydroxyurea has proven clinical efficacy in patients with sickle cell disease. Potential mechanisms for the beneficial effects include fetal hemoglobin induction and the reduction of cell adhesive properties, inflammation and hypercoagulability. Using a murine model of sickle cell disease in which fetal hemoglobin induction does not occur, we evaluated whether hydroxyurea administration would still yield improvements in hematologic parameters and reduce end-organ damage. Animals given a maximally tolerated dose of hydroxyurea that resulted in significant reductions in the neutrophil and platelet counts showed no improvement in hemolytic anemia and end-organ damage compared to control mice. In contrast, animals having high levels of fetal hemoglobin due to gene transfer with a gamma-globin lentiviral vector showed correction of anemia and organ damage. These data suggest that induction of fetal hemoglobin by hydroxyurea is an essential mechanism for its clinical benefits.
摘要
羟基脲已被证明对镰状细胞病患者具有临床疗效。其有益作用的潜在机制包括诱导胎儿血红蛋白生成以及降低细胞黏附特性、减轻炎症和高凝状态。我们利用镰状细胞病的小鼠模型进行研究,该模型不会诱导胎儿血红蛋白生成,旨在评估羟脲给药是否仍能改善血液学参数并减少终末器官损伤。接受最大耐受剂量羟脲治疗的动物,其中性粒细胞和血小板计数显著降低,但与对照小鼠相比,溶血性贫血和终末器官损伤无改善。相比之下,由于用γ-珠蛋白慢病毒载体进行基因转移而具有高胎儿血红蛋白水平的动物,其贫血和器官损伤得到纠正。这些数据表明,羟脲诱导胎儿血红蛋白生成是其临床获益的一个重要机制。
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