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小鼠红白血病(Friend)细胞的分化:红细胞生成的体外模型。

Differentiation of murine erythroleukemic (Friend) cells: an in vitro model of erythropoiesis.

作者信息

Orkin S H

出版信息

In Vitro. 1978 Jan;14(1):146-54. doi: 10.1007/BF02618181.

Abstract

Normal erythropoiesis involves differentiation of uncommitted stem cells through committed erythroid precursors into cells specialized for hemoglobin synthesis. Several aspects of this developmental sequence may be studied in murine erythroleukemic cells infected with Friend virus complex. These cells are arrested at the proerythroblast stage, yet capable of continuous growth in vitro. Maturation along an erythroid pathway is induced after treatment with a variety of agents (e.g. dimethylsulfoxide, butyric acid, hemin, ouabain). Following induction, the cells morphologically resemble normoblasts, accumulate globin mRNAs and strain-specific globins, increase heme synthesis and acquire erythrocyte membrane antigens. Cloned populations of erythroleukemic cells mature in a nonhomogeneous fashion upon induction, indicative of a stochastic response in the inductive process. This "probability of differentiation" phenotype is formally analogous to stem cell development in which hematopoietic precursor cells form a constant, dividing population from which cells are continuously maturing. Although the sequence of events involved in triggering differentiation is uncertain, cloning and cell hybridization experiments demonstrate that this phenotype is under rather stable genetic (or epigenetic) control. Recent molecular analysis shows that induced differentiation is accompanied by transcriptional activation of the globin genes rather than posttranscriptional stabilization of the globin RNAs. Further application of cellular, molecular and genetic approaches in this system may help to define specific control mechanisms in erythroid development.

摘要

正常的红细胞生成涉及未定向干细胞通过定向红细胞前体分化为专门用于血红蛋白合成的细胞。在感染了弗氏病毒复合体的小鼠红白血病细胞中,可以研究这一发育序列的几个方面。这些细胞停滞在早幼红细胞阶段,但能够在体外持续生长。用多种试剂(如二甲基亚砜、丁酸、血红素、哇巴因)处理后,可诱导细胞沿红细胞途径成熟。诱导后,细胞在形态上类似于正成红细胞,积累珠蛋白mRNA和菌株特异性珠蛋白,增加血红素合成并获得红细胞膜抗原。红白血病细胞的克隆群体在诱导后以非均匀方式成熟,这表明诱导过程中存在随机反应。这种“分化概率”表型在形式上类似于干细胞发育,其中造血前体细胞形成一个不断分裂的群体,细胞从中不断成熟。虽然触发分化所涉及的事件顺序尚不确定,但克隆和细胞杂交实验表明,这种表型受到相当稳定的遗传(或表观遗传)控制。最近的分子分析表明,诱导分化伴随着珠蛋白基因的转录激活,而不是珠蛋白RNA的转录后稳定。在这个系统中进一步应用细胞、分子和遗传方法可能有助于确定红细胞发育中的特定控制机制。

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