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用c-myc逆转录病毒衍生的小鼠红细胞系对白血病抑制因子、促红细胞生成素和白细胞介素3有反应。

Murine erythroid cell lines derived with c-myc retroviruses respond to leukemia-inhibitory factor, erythropoietin, and interleukin 3.

作者信息

Cory S, Maekawa T, McNeall J, Metcalf D

机构信息

Walter and Eliza Hall Institute of Medical Research, Royal Melbourne Hospital, Victoria, Australia.

出版信息

Cell Growth Differ. 1991 Mar;2(3):165-72.

PMID:1905566
Abstract

The transforming potential of the c-myc gene is shown here, for the first time, to include murine erythroid cells. Continuously growing cell lines were reproducibly generated by infection of day 13 CBA fetal liver cells with novel recombinant c-myc retroviruses. By cytostaining, most cells resembled early erythroblasts, but certain lines also contained significant numbers of hemoglobinized cells. RNA analysis revealed substantial expression of the genes encoding beta-globin and the erythroid-specific transcription factor GF-1. Although apparently immortal, the lines were not initially transplantable. Thus, constitutive myc expression in early erythroid cells can enhance their self-renewal capacity but is insufficient to fully transform them. The cell lines proliferated without the addition of exogenous factors, but their clonogenicity in semisolid medium was enhanced in the presence of erythropoietin, interleukin 3, and/or leukemia-inhibitory factor. In combination with either interleukin 3 or erythropoietin, leukemia-inhibitory factor also facilitated differentiation of certain lines. These results suggest that leukemia-inhibitory factor may have a previously unsuspected role in the regulation of erythropoiesis and could be considered as a possible therapeutic agent for the clinical management of erythroleukemia.

摘要

c-myc基因的转化潜能在此首次显示包括鼠类红系细胞。通过用新型重组c-myc逆转录病毒感染第13天的CBA胎肝细胞,可重复性地产生持续生长的细胞系。通过细胞染色,大多数细胞类似于早期成红细胞,但某些细胞系也含有大量血红蛋白化细胞。RNA分析显示编码β-珠蛋白和红系特异性转录因子GF-1的基因有大量表达。尽管这些细胞系显然具有永生性,但最初不能移植。因此,早期红系细胞中组成型myc表达可增强其自我更新能力,但不足以使其完全转化。这些细胞系在不添加外源性因子的情况下增殖,但在促红细胞生成素、白细胞介素3和/或白血病抑制因子存在时,它们在半固体培养基中的克隆形成能力增强。白血病抑制因子与白细胞介素3或促红细胞生成素联合使用时,也促进了某些细胞系的分化。这些结果表明,白血病抑制因子可能在红细胞生成的调节中具有先前未被怀疑的作用,并且可被视为红白血病临床治疗的一种可能治疗剂。

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