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Transient accumulation phosphorylation and changes in the oligomerization of Hsp27 during retinoic acid-induced differentiation of HL-60 cells: possible role in the control of cellular growth and differentiation

机译:维甲酸诱导HL-60细胞分化过程中Hsp27的瞬时积累磷酸化和寡聚化变化:在控制细胞生长和分化中的可能作用

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摘要

Expression of the mammalian small stress protein Hsp27 has been increasingly linked to cell growth regulation and differentiation. Hsp27 is a phosphoprotein which forms oligomers with native sizes ranging between 100 and 800 kDa. We have examined the fate of Hsp27 transiently expressed during the retinoic acid (tRA)-induced granulocytic differentiation of human leukemic HL-60 cells. We show that tRA, in addition to its effects on Hsp27 accumulation and phosphorylation, transiently increased the oligomerization state of this protein. While Hsp27 phosphorylation by tRA is an early phenomenon that takes place before cellular growth is altered, the redistribution of Hsp27 oligomers occurred later and concomitantly with the maximal accumulation of this protein. Hence, complex regulations of Hsp27 are induced by tRA which suggest that this protein plays a role in the pathway through which retinoids exert their effects. To approach Hsp27 function during HL-60 cell differentiation, experiments aimed at reducing the cellular content of this protein were performed by transiently inhibiting Hsp27 mRNA translation by a specific anti-sense oligonucleotide. This process, which decreased the basal level of Hsp27 by about 40%, did not interfere with the growth of undifferentiated HL-60 cells. In contrast, a decreased level of Hsp27 diminished the differentiation-mediated down-regulation of cell growth and altered some morphological changes induced by this retinoid. These results suggest that Hsp27 is a mediator of granulocytic differentiation.
机译:哺乳动物小应激蛋白Hsp27的表达已越来越多地与细胞生长调节和分化相关。 Hsp27是一种磷蛋白,可形成天然大小在100至800 kDa之间的寡聚体。我们已经检查了视黄酸(tRA)诱导人类白血病HL-60细胞的粒细胞分化过程中瞬时表达的Hsp27的命运。我们显示tRA,除了其对Hsp27积累和磷酸化的影响,暂时增加了该蛋白的寡聚状态。虽然通过tRA进行的Hsp27磷酸化是在细胞生长发生改变之前发生的早期现象,但Hsp27寡聚体的重新分布较晚发生,并且伴随该蛋白质的最大积累。因此,tRA诱导了Hsp27的复杂调控,表明该蛋白在类维生素A发挥作用的途径中起作用。为了在HL-60细胞分化过程中达到Hsp27的功能,旨在通过特异性反义寡核苷酸瞬时抑制Hsp27 mRNA翻译来进行旨在降低该蛋白细胞含量的实验。该过程将Hsp27的基础水平降低了约40%,但并未干扰未分化的HL-60细胞的生长。相反,降低的Hsp27水平减少了分化介导的细胞生长下调,并改变了这种类维生素A诱导的一些形态变化。这些结果表明,Hsp27是粒细胞分化的介质。

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