Alcalay M, Tomassoni L, Colombo E, Stoldt S, Grignani F, Fagioli M, Szekely L, Helin K, Pelicci P G
Department of Experimental Oncology, European Institute of Oncology, Milan, Italy.
Mol Cell Biol. 1998 Feb;18(2):1084-93. doi: 10.1128/MCB.18.2.1084.
PML is a nuclear protein with growth-suppressive properties originally identified in the context of the PML-retinoic acid receptor alpha (RAR alpha) fusion protein of acute promyelocytic leukemia. PML localizes within distinct nuclear structures, called nuclear bodies, which are disrupted by the expression of PML-RAR alpha. We report that PML colocalizes with the nonphosphorylated fraction of the retinoblastoma protein (pRB) within nuclear bodies and that pRB is delocalized by PML-RAR alpha expression. Both PML and PML-RAR alpha form complexes with the nonphosphorylated form of pRB in vivo, and they interact with the pocket region of pRB. The regions of PML and PML-RAR alpha involved in pRB binding differ; in fact, the B boxes and the C-terminal region of PML, the latter of which is not present in PML-RAR alpha, are essential for the formation of stable complexes with pRB. Functionally, PML abolishes activation of glucocorticoid receptor-regulated transcription by pRB, whereas PML-RAR alpha further increases it. Our results suggest that PML may be part of transcription-regulatory complexes and that the oncogenic potential of the PML-RAR alpha protein may derive from the alteration of PML-regulated transcription.
早幼粒细胞白血病蛋白(PML)是一种具有生长抑制特性的核蛋白,最初是在急性早幼粒细胞白血病的PML - 维甲酸受体α(RARα)融合蛋白的背景下被鉴定出来的。PML定位于独特的核结构内,称为核体,而PML - RARα的表达会破坏这些核体。我们报告称,PML在核体内与视网膜母细胞瘤蛋白(pRB)的非磷酸化部分共定位,并且pRB会因PML - RARα的表达而发生定位改变。在体内,PML和PML - RARα均与非磷酸化形式的pRB形成复合物,并且它们与pRB的口袋区域相互作用。PML和PML - RARα中参与与pRB结合的区域不同;实际上,PML的B框和C末端区域(后者不存在于PML - RARα中)对于与pRB形成稳定复合物至关重要。在功能上,PML消除了pRB对糖皮质激素受体调节转录的激活作用,而PML - RARα则进一步增强了这种激活作用。我们的结果表明,PML可能是转录调节复合物的一部分,并且PML - RARα蛋白的致癌潜力可能源于PML调节的转录改变。