首页> 外文期刊>Genes, Chromosomes and Cancer >Haploinsufficiency and reduced expression of genes localized to the 8p chromosomal region in human prostate tumors.
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Haploinsufficiency and reduced expression of genes localized to the 8p chromosomal region in human prostate tumors.

机译:在人类前列腺肿瘤中,单倍剂量不足和定位于8p染色体区域的基因表达降低。

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摘要

Cytogenetic and molecular studies have suggested that deletion or rearrangement of sequences that map to the short arm of chromosome 8 may be permissive for tumorigenesis in several organ systems, and in human prostate tumors in particular. In this study, we hypothesized that genes deleted for one copy and localized to the 8p chromosomal region may be transcriptionally down-regulated or ablated in affected human prostate tumor tissues. To test this hypothesis, we used cDNA microarray analysis to determine the transcriptional profiles for 259 transcribed sequences mapping to the 8p chromosomal region for seven human prostate tumor xenografts, completely characterized for numerical and structural alterations on chromosome 8, and five normal human prostate tissues. These experiments identified 33 genes differentially expressed between normal and malignant prostate tissues, the majority of which (28/33, 85%) were transcriptionally down-regulated in malignant compared to normal human prostate tissues. Thesefindings, that haploinsufficiency and transcriptional down-regulation for genes mapping to 8p are largely coincident in human prostate tumors, should provide a powerful tool for the identification of tumor-suppressor genes associated with human prostate cancer initiation and progression.
机译:细胞遗传学和分子学研究表明,映射到8号染色体短臂的序列的缺失或重排可能允许在多个器官系统中发生肿瘤,特别是在人类前列腺肿瘤中。在这项研究中,我们假设在受影响的人前列腺肿瘤组织中,被删除一个拷贝并位于8p染色体区域的基因可能在转录上被下调或消除。为了检验该假设,我们使用cDNA微阵列分析来确定259个转录序列的转录谱,这些序列映射到7个人类前列腺肿瘤异种移植物的8p染色体区域,完全表征了8号染色体和5个正常人类前列腺组织的数字和结构改变。这些实验确定了在正常和恶性前列腺组织之间差异表达的33个基因,与正常人的前列腺组织相比,其中的大多数(28 / 33,85%)在恶性肿瘤中转录下调。这些发现,映射到8p的基因的单倍剂量不足和转录下调在人类前列腺肿瘤中大体上是重合的,应该为鉴定与人类前列腺癌的发生和发展相关的肿瘤抑制基因提供有力的工具。

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