维甲酸和环磷酸腺苷诱导的维甲酸X受体(RXRα)及其RARα和PML-RARα伴侣的差异变化区分了成熟敏感和耐药的t(15;17)早幼粒细胞白血病NB4细胞。
Differential changes of retinoid-X-receptor (RXR alpha) and its RAR alpha and PML-RAR alpha partners induced by retinoic acid and cAMP distinguish maturation sensitive and resistant t(15;17) promyelocytic leukemia NB4 cells.
作者信息
Duprez E, Lillehaug J R, Gaub M P, Lanotte M
机构信息
INSERM U-301, Génétique Moléculaire et Cellulaire des Leucémies, Centre G. Hayem, Hôpital Saint-Louis, Paris, France.
出版信息
Oncogene. 1996 Jun 6;12(11):2443-50.
The expression of retinoid receptors (RXRalpha, RARalpha and the chimeric form PML-RARalpha) was analysed both at the mRNA and protein level in the maturation sensitive NB4 and resistant NB4-R1 cell lines of t(15;17) promyelocytic leukemia (APL). All-trans RA and cAMP which show synergistic activity in inducing maturation of NB4 cells and maturation triggering of the RA 'primed' NB4-R1 resistant cells, distinctly modulate RXRalpha, RARalpha and PML-RARalpha mRNA. In the NB4 and NB4-R1 cells, RXRalpha mRNA was downregulated by RA, but only in RA-primed NB4-R1 cells a release from RXRalpha mRNA downregulation was obtained by cAMP treatment. RXRalpha protein (53 kDa) was decreased to the western-blot detection limit (97.5%) by RA in NB4 cells, but in NB4-R1 cells although it was frankly decreased (85%), the signal for RXRalpha protein remained very significant. More importantly, while cAMP slightly upregulated RXRalpha protein in RA-treated NB4 cells, it caused an increase of RXRalpha protein in RA-treated NB4-R1 cells bringing RXRalpha to the initial control level. RXRalpha partners in heterodimers (PML-RARalpha, RARalpha) were also analysed. In contrast to RXRalpha, RARalpha and PML-RARalpha mRNA were not modulated by RA and/or cAMP, while significant changes were observed at the protein levels. A putatively phosphorylated form of RARalpha (52 kDa) decreased during maturation of NB4 cells, but was unchanged in resistant NB4-R1 cells. Conversely, while PML-RARalpha remained stable during RA-induced NB4 maturation, RA treatment which failed to induce maturation of NB4-R1 cells significantly down-regulated the chimeric receptor (120 kDa). These differences most likely results from translational and post-translational regulation. This work reveals complex pattern of subtle changes at the protein level distinguishing RA-sensitive and RA-resistant cells. Our data show that the RA-cAMP synergistic effect on NB4 cell maturation and cooperation in triggering maturation of RA-primed NB4-R1 cells operate changes in the RXR/PML-RARalpha ratio which are both favouring RXRalpha. In both cell lines, variations of PML-RARalpha and RXRalpha may result in a decrease in the formation of the PML-RARalpha/RXRalpha heterodimers which are supposed involved in the block of maturation. This may prove crucial to embark cells on maturation.
在t(15;17)早幼粒细胞白血病(APL)的成熟敏感NB4和耐药NB4-R1细胞系中,从mRNA和蛋白质水平分析了类视黄醇受体(RXRα、RARα和嵌合形式PML-RARα)的表达。全反式维甲酸(ATRA)和环磷酸腺苷(cAMP)在诱导NB4细胞成熟以及触发维甲酸“预刺激”的耐药NB4-R1细胞成熟方面具有协同活性,它们可显著调节RXRα、RARα和PML-RARα的mRNA。在NB4和NB4-R1细胞中,维甲酸可下调RXRα mRNA,但仅在维甲酸预刺激的NB4-R1细胞中,cAMP处理可解除RXRα mRNA的下调。在NB4细胞中,维甲酸可将RXRα蛋白(53 kDa)降至蛋白质印迹检测下限(97.5%),但在NB4-R1细胞中,尽管其明显降低(85%),RXRα蛋白信号仍非常显著。更重要的是,虽然cAMP在维甲酸处理的NB4细胞中轻微上调RXRα蛋白,但在维甲酸处理的NB4-R1细胞中却使其增加,使RXRα恢复到初始对照水平。还分析了异二聚体中的RXRα伴侣(PML-RARα、RARα)。与RXRα不同,RARα和PML-RARα的mRNA不受维甲酸和/或cAMP的调节,但在蛋白质水平观察到显著变化。一种假定的磷酸化形式的RARα(52 kDa)在NB4细胞成熟过程中减少,但在耐药的NB4-R1细胞中保持不变。相反,虽然PML-RARα在维甲酸诱导的NB4成熟过程中保持稳定,但未能诱导NB4-R1细胞成熟的维甲酸处理却显著下调了嵌合受体(120 kDa)。这些差异很可能源于翻译和翻译后调控。这项工作揭示了在蛋白质水平上区分维甲酸敏感和耐药细胞的复杂细微变化模式。我们的数据表明,维甲酸-环磷酸腺苷对NB4细胞成熟的协同作用以及在触发维甲酸预刺激的NB4-R1细胞成熟中的协同作用,导致RXR/PML-RARα比值发生变化,这两者都有利于RXRα。在这两种细胞系中,PML-RARα和RXRα的变化可能导致PML-RARα/RXRα异二聚体形成减少,而这种异二聚体被认为与成熟阻滞有关。这可能对促使细胞成熟至关重要。
Zotero 插件