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Induction of erythroid differentiation and increased globin mRNA production with furocoumarins and their photoproducts

机译:呋喃香豆素及其光产物诱导红系分化并增加球蛋白mRNA的产生

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Differentiation-therapy is an important approach in the treatment of cancer, as in the case of erythroid induction in chronic myelogenous leukemia. Moreover, an important therapeutic strategy for treating beta-thalassemia and sickle-cell anemia could be the use of drugs able to induce erythroid differentiation and fetal hemoglobin (HbF) accumulation: in fact, the increased production of this type of hemoglobin can reduce the clinical symptoms and the frequency of transfusions. An important class of erythroid differentiating compounds and HbF inducers is composed by DNA-binding chemotherapeutics: however, they are not used in most instances considering their possible devastating side effects. In this contest, we approached the study of erythrodifferentiating properties of furocoumarins. In fact, upon UV-A irradiation, they are able to covalently bind DNA. Thus, the erythrodifferentiation activity of some linear and angular furocoumarins was evaluated in the experimental K562 cellular model system. Quantitative real-time reverse transcription polymerase-chain reaction assay was employed to evaluate the accumulation of different globin mRNAs. The results demonstrated that both linear and angular furocoumarins are strong inducers of erythroid differentiation of K562 cells. From a preliminary screening, we selected the most active compounds and investigated the role of DNA photodamage in their erythroid inducing activity and mechanism of action. Moreover, some cytofluorimetric experiments were carried out to better study cell cycle modifications and the mitochondrial involvement. A further development of the work was carried out studying the erythroid differentiation of photolysis products of these molecules. 5,5′-Dimethylpsoralen photoproducts induced an important increase in γ-globin gene transcription in K562 cells.
机译:分化疗法是治疗癌症的重要方法,例如在慢性粒细胞性白血病中类红细胞诱导的情况下。此外,治疗β地中海贫血和镰状细胞性贫血的重要治疗策略可能是使用能够诱导类红细胞分化和胎儿血红蛋白(HbF)积累的药物:实际上,这类血红蛋白产量的增加可以减少临床症状和输血频率。一类重要的类红细胞分化化合物和HbF诱导剂由结合DNA的化学疗法组成:但是,考虑到其可能的破坏性副作用,在大多数情况下不使用它们。在本次比赛中,我们进行了呋喃香豆素的红血球微分特性研究。实际上,在UV-A照射下,它们能够共价结合DNA。因此,在实验性K562细胞模型系统中评估了一些线性和角型呋喃香豆素的红细胞分化活性。实时定量逆转录聚合酶链反应法用于评估不同球蛋白mRNA的积累。结果表明,线性和有角的呋喃香豆素都是K562细胞类红细胞分化的强诱导剂。通过初步筛选,我们选择了活性最高的化合物,并研究了DNA光损伤在类胡萝卜素诱导活性和作用机理中的作用。此外,进行了一些细胞荧光实验,以更好地研究细胞周期修饰和线粒体参与。研究这些分子的光解产物的红系分化的工作进行了进一步发展。 5,5'-二甲基补骨脂素光产物在K562细胞中诱导了γ-珠蛋白基因转录的重要增加。

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