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首页> 外文期刊>Human Molecular Genetics >Retention of imprinting of the human apoptosis-related gene TSSC3 in human brain tumors.
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Retention of imprinting of the human apoptosis-related gene TSSC3 in human brain tumors.

机译:在人类脑肿瘤中保留人类凋亡相关基因TSSC3的印迹。

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Genomic imprinting is the result of a gamete-specific modification leading to parental origin-specific gene expression in somatic cells of the offspring. Several embryonal tumors show loss of imprinting of genes clustered in human chromosome 11p15.5, an important tumor suppressor gene region, harboring several normally imprinted genes. TSSC3, a gene homologous to mouse TDAG51, implicated in Fas-mediated apoptosis, is also located in this region between hNAP2 and p57 (KIP2). TSSC3 is the first apoptosis-related gene found to be imprinted in placenta, liver and fetal tissues where it is expressed from the maternal allele in normal human development. This study investigated the imprinting status of TSSC3 in human normal, adult brain and in human neuroblastomas, medulloblastomas and glioblastomas. A polymorphism in exon 1 at position 54 was used to analyze the allelic expression of the TSSC3 gene by a primer oligo base extension (PROBE) assay using matrix-assisted laser desorption ionization time-of-flight mass spectrometry (MALDI-TOF MS). We found that the TSSC3 gene is not imprinted in human normal, adult brain and blood. In contrast, strong allelic bias resembling imprinting could be detected in most examined tumor specimens. The results demonstrate for the first time that the tumors under investigation are associated with a retention of imprinting of a potential growth inhibitory gene.
机译:基因组印记是配子特异性修饰的结果,导致后代体细胞中父母起源特异性基因表达。几个胚胎肿瘤显示出在人类染色体11p15.5(一个重要的抑癌基因区域)中聚集的基因的印记丢失,其中隐含了几个正常印记的基因。 TSSC3,与小鼠TDAG51同源的基因,与Fas介导的细胞凋亡有关,也位于hNAP2和p57(KIP2)之间的此区域。 TSSC3是第一个凋亡相关基因,被发现印在胎盘,肝脏和胎儿组织中,在正常人的发育中从母体等位基因表达。这项研究调查了TSSC3在人正常,成年大脑以及人神经母细胞瘤,髓母细胞瘤和胶质母细胞瘤中的印迹状态。第54位外显子1的多态性用于通过基质辅助激光解吸电离飞行时间质谱(MALDI-TOF MS)的引物寡碱基延伸(PROBE)分析来分析TSSC3基因的等位基因表达。我们发现,TSSC3基因未在人类正常,成年大脑和血液中留下印记。相反,在大多数检查过的肿瘤标本中可以检测到类似印迹的强等位基因偏倚。结果首次证明所研究的肿瘤与潜在的生长抑制基因的印迹保留有关。

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