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人类细胞中的小多分散环状DNA(spcDNA):与基因组不稳定的关联。

Small polydispersed circular DNA (spcDNA) in human cells: association with genomic instability.

作者信息

Cohen S, Regev A, Lavi S

机构信息

Department of Cell Research and Immunology, The George S Wise Faculty of Life Sciences, Tel-Aviv University, Israel.

出版信息

Oncogene. 1997 Feb 27;14(8):977-85. doi: 10.1038/sj.onc.1200917.

Abstract

Small Polydispersed Circular DNA (spcDNA) was suggested to be associated with genetically unstable cells. However, until now, qualitative and quantitative research has been limited due to the lack of efficient methods for detection and analysis. We developed a two-dimensional (2-D) neutral-neutral gel electrophoresis assay for the identification, characterisation and quantitation of spcDNA. Using this method, we established the relation of spcDNA to genetic and induced genomic instability in human cells, both in vitro and in vivo. Enhanced amounts of spcDNA were found in genetically unstable cells and tissues. spcDNA was detected in a tumor cell-line (HeLa) and in tumor tissue (colon carcinoma) as well as in fibroblasts derived from patients suffering from the genomic instability disease, Fanconi's Anemia. We failed to detect spcDNA in the genetically stable normal human fibroblasts. However, following treatment with the initiating carcinogen MNNG, an induction of spcDNA was observed. The level of spcDNA was quantified according to mitochondrial DNA (mtDNA) standards. In light of these findings, we discuss the possible role of spcDNA as a marker and an enhancer of genomic instability.

摘要

小多分散环状DNA(spcDNA)被认为与基因不稳定细胞有关。然而,直到现在,由于缺乏有效的检测和分析方法,定性和定量研究一直受到限制。我们开发了一种二维(2-D)中性-中性凝胶电泳分析法,用于spcDNA的鉴定、表征和定量。使用这种方法,我们在体外和体内建立了spcDNA与人类细胞中遗传和诱导基因组不稳定的关系。在基因不稳定的细胞和组织中发现了spcDNA的量增加。在肿瘤细胞系(HeLa)、肿瘤组织(结肠癌)以及患有基因组不稳定疾病范可尼贫血患者的成纤维细胞中检测到了spcDNA。我们未能在基因稳定的正常人成纤维细胞中检测到spcDNA。然而,在用起始致癌物MNNG处理后,观察到spcDNA的诱导。根据线粒体DNA(mtDNA)标准对spcDNA的水平进行了定量。鉴于这些发现,我们讨论了spcDNA作为基因组不稳定的标志物和增强剂的可能作用。

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