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Ras信号在小鼠胎肝细胞红系分化中的作用:基于流式细胞术的新型培养系统的功能分析

Role of Ras signaling in erythroid differentiation of mouse fetal liver cells: functional analysis by a flow cytometry-based novel culture system.

作者信息

Zhang Jing, Socolovsky Merav, Gross Alec W, Lodish Harvey F

机构信息

Whitehead Institute for Biomedical Research, 9 Cambridge Center, Cambridge, MA 02142, USA.

出版信息

Blood. 2003 Dec 1;102(12):3938-46. doi: 10.1182/blood-2003-05-1479. Epub 2003 Aug 7.

Abstract

Ras signaling plays an important role in erythropoiesis. Its function has been extensively studied in erythroid and nonerythroid cell lines as well as in primary erythroblasts, but inconclusive results using conventional erythroid colony-forming unit (CFU-E) assays have been obtained concerning the role of Ras signaling in erythroid differentiation. Here we describe a novel culture system that supports terminal fetal liver erythroblast proliferation and differentiation and that closely recapitulates erythroid development in vivo. Erythroid differentiation is monitored step by step and quantitatively by a flow cytometry analysis; this analysis distinguishes CD71 and TER119 double-stained erythroblasts into different stages of differentiation. To study the role of Ras signaling in erythroid differentiation, different H-ras proteins were expressed in CFU-E progenitors and early erythroblasts with the use of a bicistronic retroviral system, and their effects on CFU-E colony formation and erythroid differentiation were analyzed. Only oncogenic H-ras, not dominant-negative H-ras, reduced CFU-E colony formation. Analysis of infected erythroblasts in our newly developed system showed that oncogenic H-ras blocks terminal erythroid differentiation, but not through promoting apoptosis of terminally differentiated erythroid cells. Rather, oncogenic H-ras promotes abnormal proliferation of CFU-E progenitors and early erythroblasts and supports their erythropoietin (Epo)-independent growth.

摘要

Ras信号传导在红细胞生成中起重要作用。其功能已在红系和非红系细胞系以及原代成红细胞中得到广泛研究,但关于Ras信号传导在红系分化中的作用,使用传统的红系集落形成单位(CFU-E)检测方法得到的结果并不确定。在此,我们描述了一种新型培养系统,该系统支持终末胎肝成红细胞的增殖和分化,并且能紧密模拟体内红系发育过程。通过流式细胞术分析逐步且定量地监测红系分化;该分析可将CD71和TER119双染的成红细胞区分到不同的分化阶段。为了研究Ras信号传导在红系分化中的作用,利用双顺反子逆转录病毒系统在CFU-E祖细胞和早期成红细胞中表达不同的H-ras蛋白,并分析它们对CFU-E集落形成和红系分化的影响。只有致癌性H-ras,而非显性负性H-ras,会减少CFU-E集落形成。在我们新开发的系统中对受感染的成红细胞进行分析表明,致癌性H-ras会阻断终末红系分化,但并非通过促进终末分化红系细胞的凋亡。相反,致癌性H-ras会促进CFU-E祖细胞和早期成红细胞的异常增殖,并支持它们不依赖促红细胞生成素(Epo)的生长。

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