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在携带t(6;7)(q23;q36)的白血病细胞系GDM-1中,未易位的HLXB9等位基因的核重定位

Nuclear Repositioning of the Non-Translocated HLXB9 Allele in the Leukaemia Cell Line GDM-1 Harbouring a t(6;7)(q23;q36).

作者信息

Federico Concetta, Leotta Claudia G, Bruno Francesca, Longo Anna M, Owoka Temitayo, Tosi Sabrina, Saccone Salvatore

机构信息

Dipartimento di Scienze Biologiche, Geologiche e Ambientali, University of Catania, Catania, Italy.

出版信息

Cytogenet Genome Res. 2017;153(1):10-17. doi: 10.1159/000480745. Epub 2017 Sep 29.

Abstract

Transcriptionally active and inactive topologically associated domains (TADs) occupy different areas in the cell nucleus, and chromosomal rearrangements relocating TADs could determine ectopic expression of the repositioned genes. In this study, we investigated the HLXB9 gene in a myeloid leukaemia cell line, GDM-1, known to harbour a rearrangement involving chromosome 7 with a breakpoint distal to HLXB9, highly expressed in these cells. We used FISH to target the regions involved in the translocation and to distinguish the translocated chromosome from the non-translocated one in interphase nuclei. Two-dimensional analysis of the interphase FISH data indicated that the 2 HLXB9 alleles had a different localisation in the cell nuclei, with the translocated allele consistently positioned in the nuclear periphery and the normal one in the more internal portion of the nucleus, known as the transcriptionally active compartment. Our data may indicate that HLXB9 transcripts in the GDM-1 cell line do not arise from the allele located in rearranged chromosome 7, suggesting that regulation of gene expression in cancer cells harbouring chromosomal translocations might be more complex than previously thought, paving the path to further investigations on mechanisms of gene expression.

摘要

转录活跃和不活跃的拓扑相关结构域(TADs)在细胞核中占据不同区域,而重新定位TADs的染色体重排可能决定重新定位基因的异位表达。在本研究中,我们在一种髓系白血病细胞系GDM-1中研究了HLXB9基因,已知该细胞系存在涉及7号染色体的重排,断点位于HLXB9远端,且该基因在这些细胞中高表达。我们使用荧光原位杂交(FISH)来靶向易位涉及的区域,并在间期核中区分易位染色体和未易位染色体。对间期FISH数据的二维分析表明,两个HLXB9等位基因在细胞核中的定位不同,易位等位基因始终位于核周边,而正常等位基因位于核的更内部区域,即转录活跃区室。我们的数据可能表明,GDM-1细胞系中的HLXB9转录本并非来自位于重排7号染色体上的等位基因,这表明携带染色体重排的癌细胞中的基因表达调控可能比以前认为的更为复杂,为进一步研究基因表达机制铺平了道路。

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