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红系分化的调控:AEV 和 S13 转化细胞中阴离子转运蛋白与膜骨架外周成分的异步表达

Control of erythroid differentiation: asynchronous expression of the anion transporter and the peripheral components of the membrane skeleton in AEV- and S13-transformed cells.

作者信息

Woods C M, Boyer B, Vogt P K, Lazarides E

出版信息

J Cell Biol. 1986 Nov;103(5):1789-98. doi: 10.1083/jcb.103.5.1789.

Abstract

Chicken erythroblasts transformed with avian erythroblastosis virus or S13 virus provide suitable model systems with which to analyze the maturation of immature erythroblasts into erythrocytes. The transformed cells are blocked in differentiation at around the colony-forming unit-erythroid stage of development but can be induced to differentiate in vitro. Analysis of the expression and assembly of components of the membrane skeleton indicates that these cells simultaneously synthesize alpha-spectrin, beta-spectrin, ankyrin, and protein 4.1 at levels that are comparable to those of mature erythroblasts. However, they do not express any detectable amounts of anion transporter. The peripheral membrane skeleton components assemble transiently and are subsequently rapidly catabolized, resulting in 20-40-fold lower steady-state levels than are found in maturing erythrocytes. Upon spontaneous or chemically induced terminal differentiation of these cells expression of the anion transporter is initiated with a concommitant increase in the steady-state levels of the peripheral membrane-skeletal components. These results suggest that during erythropoiesis, expression of the peripheral components of the membrane skeleton is initiated earlier than that of the anion transporter. Furthermore, they point a key role for the anion transporter in conferring long-term stability to the assembled erythroid membrane skeleton during terminal differentiation.

摘要

用禽成红细胞增多症病毒或S13病毒转化的鸡成红细胞提供了合适的模型系统,用于分析未成熟成红细胞向红细胞的成熟过程。转化细胞在发育的集落形成单位-红细胞阶段左右的分化过程中被阻断,但可在体外诱导分化。对膜骨架成分的表达和组装分析表明,这些细胞同时合成α-血影蛋白、β-血影蛋白、锚蛋白和蛋白4.1,其水平与成熟成红细胞相当。然而,它们不表达任何可检测量的阴离子转运蛋白。外周膜骨架成分短暂组装,随后迅速分解代谢,导致稳态水平比成熟红细胞低20-40倍。在这些细胞自发或化学诱导的终末分化时,阴离子转运蛋白的表达开始,同时外周膜骨架成分的稳态水平增加。这些结果表明,在红细胞生成过程中,膜骨架外周成分的表达比阴离子转运蛋白的表达更早开始。此外,它们指出了阴离子转运蛋白在终末分化过程中赋予组装好的红细胞膜骨架长期稳定性方面的关键作用。

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