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急性早幼粒细胞白血病的t(15;17)易位将维甲酸受体α基因与一个新的转录位点融合。

The t(15;17) translocation of acute promyelocytic leukaemia fuses the retinoic acid receptor alpha gene to a novel transcribed locus.

作者信息

de Thé H, Chomienne C, Lanotte M, Degos L, Dejean A

机构信息

Unité de Recombinaison et Expression Génétique, INSERM U.163, CNRS URA 271, Institut Pasteur, Paris, France.

出版信息

Nature. 1990 Oct 11;347(6293):558-61. doi: 10.1038/347558a0.

Abstract

Retinoic acid is a vitamin A derivative with striking effects on development and cell differentiation. Several nuclear retinoic acid receptors (RARs), acting as ligand-inducible transcription factors, have been characterized and indirect evidence suggests that they have distinct roles. One of the most intriguing properties of retinoic acid is its ability to induce in vivo differentiation of acute promyelocytic leukaemia (APL) cells into mature granulocytes, leading to morphological complete remissions. Because the RAR alpha gene maps to chromosome 17q21 (ref. 14), close to the t(15;17) (q21-q11-22) translocation specifically associated with APL, we analysed RAR alpha gene structure and expression in APL cells. We report here that, in one APL-derived cell line, the RAR alpha gene has been translocated to a locus, myl, on chromosome 15, resulting in the synthesis of a myl/RAR alpha fusion messenger RNA. Using two probes located on either side of the cloned breakpoint, we have found genomic rearrangements of one or other locus in six patients out of eight, demonstrating that the RAR alpha and/or myl genes are frequently rearranged in APL and the breakpoints are clustered. These findings strongly implicate retinoic acid receptor alpha in leukaemogenesis.

摘要

维甲酸是一种维生素A衍生物,对发育和细胞分化具有显著影响。几种核维甲酸受体(RARs)作为配体诱导型转录因子已得到表征,间接证据表明它们具有不同的作用。维甲酸最引人关注的特性之一是其能够在体内诱导急性早幼粒细胞白血病(APL)细胞分化为成熟粒细胞,从而导致形态学完全缓解。由于RARα基因定位于17号染色体q21(参考文献14),靠近与APL特异性相关的t(15;17)(q21-q11-22)易位,我们分析了APL细胞中RARα基因的结构和表达。我们在此报告,在一个源自APL的细胞系中,RARα基因已易位至15号染色体上的一个位点myl,导致合成了myl/RARα融合信使RNA。使用位于克隆断点两侧的两个探针,我们在8例患者中的6例中发现了一个或另一个位点的基因组重排,表明RARα和/或myl基因在APL中经常发生重排且断点聚集。这些发现强烈提示维甲酸受体α与白血病发生有关。

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