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Mathematical modeling reveals differential effects of erythropoietin on proliferation and lineage commitment of human hematopoietic progenitors in early erythroid culture

机译:数学模型揭示了促红细胞生成素对早期红系培养物中人类造血祖细胞增殖和谱系承诺的不同影响

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摘要

Erythropoietin is essential for the production of mature erythroid cells, promoting both proliferation and survival. Whether erythropoietin and other cytokines can influence lineage commitment of hematopoietic stem and progenitor cells is of significant interest. To study lineage restriction of the common myeloid progenitor to the megakaryocyte/erythroid progenitor of peripheral blood CD34+ cells, we have shown that the cell surface protein CD36 identifies the earliest lineage restricted megakaryocyte/erythroid progenitor. Using this marker and carboxyfluorescein succinimidyl ester to track cell divisions in vitro, we have developed a mathematical model that accurately predicts population dynamics of erythroid culture. Parameters derived from the modeling of cultures without added erythropoietin indicate that the rate of lineage restriction is not affected by erythropoietin. By contrast, megakaryocyte/erythroid progenitor proliferation is sensitive to erythropoietin from the time that CD36 first appears at the cell surface. These results shed new light on the role of erythropoietin in erythropoiesis and provide a powerful tool for further study of hematopoietic progenitor lineage restriction and erythropoiesis.
机译:促红细胞生成素对于产生成熟的类红细胞至关重要,可促进增殖和存活。促红细胞生成素和其他细胞因子是否能影响造血干细胞和祖细胞的谱系定型是非常重要的。为了研究普通髓样祖细胞对外周血CD34 + 细胞的巨核细胞/红系祖细胞的谱系限制,我们发现细胞表面蛋白CD36鉴定了最早的谱系限制的巨核细胞/红系祖细胞。使用该标记物和羧基荧光素琥珀酰亚胺酯在体外追踪细胞分裂,我们已经开发出数学模型,可以准确地预测类红细胞培养的种群动态。从不添加促红细胞生成素的培养物建模中得出的参数表明,沿谱限制的速率不受促红细胞生成素的影响。相比之下,从CD36首次出现在细胞表面起,巨核细胞/类红细胞祖细胞增殖就对促红细胞生成素敏感。这些结果为促红细胞生成素在促红细胞生成中的作用提供了新的思路,并为进一步研究造血祖细胞谱系限制和促红细胞生成提供了有力的工具。

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