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首页> 外文期刊>Cellular Oncology: Analytical Cellular Pathology >Topography of Genetic Loci in Tissue Samples: Towards New Diagnostic Tool Using Interphase FISH and High-Resolution Image Analysis Techniques
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Topography of Genetic Loci in Tissue Samples: Towards New Diagnostic Tool Using Interphase FISH and High-Resolution Image Analysis Techniques

机译:组织样品中遗传基因座的拓扑:使用相间FISH和高分辨率图像分析技术的新型诊断工具

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Using single and dual colour fluorescencein situhybridisation (FISH) combined with image analysis techniques the topographic characteristics of genes and centromeres in nuclei of human colon tissue cells were investigated. The distributions of distances from the centre‐of‐nucleus to genes (centromeres) and from genes to genes (centromeres to centromeres) were studied in normal colon tissue cells found in the neighbourhood of tumour samples, in tumour cell line HT‐29 and in promyelocytic HL‐60 cell line for comparison. Our results show that the topography of genetic loci determined in 3D‐fixed cell tissue corresponds to that obtained for 2D‐fixed cells separated from the tissue. The distributions of the centre‐of‐nucleus to gene (centromere) distances and gene to gene (centromere to centromere) distances and their average values are different for various genetic loci but similar for normal colon tissue cells, HT‐29 colon tumour cell line and HL‐60 promyelocytic cell line. It suggests that the arrangement of genetic loci in cell nucleus is conserved in different types of human cells. The investigations of trisomic loci in HT‐29 cells revealed that the location of the third genetic element is not different from the location of two homologues in diploid cells. We have shown that the topographic parameters used in our experiments for different genetic elements are not tissue or tumour specific. In order to validate high‐resolution cytometry for oncology, further investigations should include more precise parameters reflecting the state of chromatin in the neighbourhood of critical oncogenes or tumour suppresser genes.
机译:使用单色和双色荧光原位杂交(FISH)与图像分析技术相结合,研究了人类结肠组织细胞核中基因和着丝粒的形貌特征。在肿瘤样本附近,HT-29细胞系和肿瘤细胞系中发现的正常结肠组织细胞中研究了从细胞核中心到基因(着丝粒)和从基因到基因(着丝粒到着丝粒)的距离分布。用于比较的早幼粒细胞HL-60细胞系。我们的结果表明,在3D固定的细胞组织中确定的遗传基因座的拓扑结构与从组织分离的2D固定的细胞所获得的拓扑结构相对应。各个遗传基因座的核中心到基因(着丝粒)距离和基因到基因(着丝粒到着丝粒)距离的分布及其平均值均不同,但对于正常结肠组织细胞HT-29结肠肿瘤细胞系而言,相似和HL-60早幼粒细胞系。这表明在不同类型的人类细胞中,基因位点在细胞核中的排列是保守的。 HT-29细胞中三体位点的研究表明,第三个遗传元件的位置与二倍体细胞中两个同源物的位置没有不同。我们已经表明,在我们的实验中,用于不同遗传因素的地形参数不是组织或肿瘤特异性的。为了验证用于肿瘤学的高分辨率细胞术,进一步的研究应包括更精确的参数,以反映关键癌基因或抑癌基因附近的染色质状态。

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