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基因组改变对转录组的影响:一项前列腺癌细胞系案例研究。

The impact of genomic alterations on the transcriptome: a prostate cancer cell line case study.

作者信息

Chaudhary J, Schmidt M

机构信息

4029D RCST, Department of Biological Sciences, Center for Cancer Research and Therapeutics Development, Clark Atlanta University, Atlanta, GA 30314, USA.

出版信息

Chromosome Res. 2006;14(5):567-86. doi: 10.1007/s10577-006-1055-4. Epub 2006 Jul 12.

Abstract

Genetic instability may lead to the loss/gain of transcriptional control. Here we investigated the effect of genomic instability, that is loss/gain of chromosomal regions on the global transcriptome of prostate cancer cell line DU145. The genomic loss/gain map obtained through BAC array-based CGH was superimposed on the dynamic transcriptome of DU145 cells treated with serum for 0 h (serum starved), 2 h and 12 h. The genomic analysis suggested that in DU145 cells: (1) chromosomal gains are prominent than losses and (2) copy number changes are associated with chromosome-specific and dynamic gene expression regulatory mechanisms. A significant proportion of the genes in the stable regions of the chromosome were up-regulated whereas a higher proportion of genes were down-regulated at 2 and 12 h in the deleted regions of the chromosomes following serum treatment. No change in expression was observed for the genes in the gained regions over a period of time. This analysis led us to propose that loss of heterozygosity leads to an overall transcriptional down-regulation that may further lead to a decrease in the expression of putative tumor suppressors. The genomic profile of DU145 is similar to pathological specimens of prostate cancer, hence the genomic/transcriptomic signature of DU145 can be used to understand the pathology of prostate cancer. It is expected that this analysis will allow a better understanding of transcriptional regulatory mechanisms in the context of genomic loss and gain and may lead to the discovery of novel oncogenes and tumor suppressors and the underlying regulatory pathways.

摘要

基因不稳定可能导致转录调控的丧失/获得。在此,我们研究了基因组不稳定,即染色体区域的缺失/获得对前列腺癌细胞系DU145的整体转录组的影响。通过基于BAC阵列的比较基因组杂交获得的基因组缺失/获得图谱被叠加到用血清处理0小时(血清饥饿)、2小时和12小时的DU145细胞的动态转录组上。基因组分析表明,在DU145细胞中:(1)染色体增加比缺失更显著;(2)拷贝数变化与染色体特异性和动态基因表达调控机制相关。染色体稳定区域中的很大一部分基因上调,而在血清处理后染色体缺失区域中,2小时和12小时时有更高比例的基因下调。在一段时间内,获得区域中的基因未观察到表达变化。该分析使我们提出,杂合性缺失导致整体转录下调,这可能进一步导致假定的肿瘤抑制因子表达降低。DU145的基因组图谱与前列腺癌的病理标本相似,因此DU145的基因组/转录组特征可用于理解前列腺癌的病理。预计该分析将有助于更好地理解基因组缺失和获得情况下的转录调控机制,并可能导致发现新的癌基因和肿瘤抑制因子以及潜在的调控途径。

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