首页> 美国卫生研究院文献>The Journal of Clinical Investigation >Mechanism of Hb F stimulation by S-stage compounds. In vitro studies with bone marrow cells exposed to 5-azacytidine, Ara-C, or hydroxyurea.
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Mechanism of Hb F stimulation by S-stage compounds. In vitro studies with bone marrow cells exposed to 5-azacytidine, Ara-C, or hydroxyurea.

机译:S-阶段化合物刺激Hb F的机制。暴露于5-氮胞苷,Ara-C或羟基脲的骨髓细胞的体外研究。

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摘要

The in vitro effect of S-stage-specific drugs on the fetal hemoglobin (Hb F) potential of erythroid precursors and progenitors was tested by exposing bone marrow cells to 5-aza-2'-deoxycytidine, Ara-C, or hydroxyurea in suspension cultures and reculturing the cells in drug-free clonal cultures. Analysis of Hb F in the erythroblasts present at the end of suspension cultures and in the erythroid colonies formed from treated progenitors showed that 1 X 10(-9)-5 X 10(-8) M 5-aza-2'-deoxycytidine produced a concentration-related increase in the proportion of Hb F-positive erythroblasts, of Hb F-positive erythroid CFU (CFUe) colonies, and at the higher doses used, an increased Hb F expression in erythroid burst-forming unit (BFUe)-derived colonies. Preincubation of bone marrow cells with Ara-C produced significant megaloblastic changes by the end of the 2-d incubation and increased the proportion of Hb F-positive erythroblasts, CFUe colonies, and e-clusters, but BFUe-derived progeny was unaffected. Hydroxyurea failed to produce significant changes in Hb F at the range of concentrations used. The data raise the possibility of more than one mechanism underlying the stimulation of Hb F by S-stage drugs.
机译:通过将骨髓细胞暴露于悬浮液中的5-氮杂2'-脱氧胞苷,Ara-C或羟基脲中,测试了S期特异性药物对类红血球前体和祖细胞的胎儿血红蛋白(Hb F)电位的体外影响。培养和在无毒克隆培养物中再培养细胞。分析悬浮培养结束时存在的成红细胞中的Hb F和由处理过的祖细胞形成的类红细胞菌落中的Hb F显示,产生了1 X 10(-9)-5 X 10(-8)M 5-aza-2'-脱氧胞苷Hb F阳性红系细胞,Hb F阳性红系CFU(CFUe)菌落的比例与浓度相关的增加,并且在使用更高剂量时,源自红系爆发形成单位(BFUe)的Hb F表达增加群落。骨髓细胞与Ara-C的预温育在2天温育结束时产生了显着的巨幼细胞变化,并增加了Hb F阳性成红细胞,CFUe集落和e-簇的比例,但BFUe衍生的后代不受影响。在所使用的浓度范围内,羟基脲未能在Hb F中产生显着变化。数据提出了由S期药物刺激Hb F的一种以上机制的可能性。

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