首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Amplified human MYC oncogenes localized to replicating submicroscopic circular DNA molecules.
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Amplified human MYC oncogenes localized to replicating submicroscopic circular DNA molecules.

机译:扩增的人类MYC癌基因位于复制的亚显微环状DNA分子上。

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摘要

Amplification of genes can sometimes be detected by molecular hybridization but not by cytogenetic methods, suggesting that in some cases the units of amplification may be too small to be detected by light microscopy. The experiments reported here investigate whether submicroscopic amplification units are present in early passages of the human tumor cell lines HL-60 and COLO 320. The results show that such cells do contain submicroscopic, extrachromosomal, supercoiled circular molecules harboring MYC genes. The molecules in HL-60 are approximately 250 kilobase pairs (kbp), while those in COLO 320 are 120-160 kbp. The extrachromosomal molecules in HL-60 are shown to replicate semiconservatively and approximately once in one cell cycle. We propose that these submicroscopic elements are precursors of double-minute chromosomes, the usual extrachromosomal manifestation of gene amplification, since both are structurally similar and replicate autonomously.
机译:有时可以通过分子杂交而不是细胞遗传学方法检测基因的扩增,这表明在某些情况下,扩增单位可能太小,无法通过光学显微镜检测到。此处报道的实验研究了人类肿瘤细胞系HL-60和COLO 320的早期传代中是否存在亚显微扩增单元。结果表明,此类细胞确实含有携带MYC基因的亚显微,染色体外,超螺旋环状分子。 HL-60中的分子约为250千碱基对(kbp),而COLO 320中的分子则为120-160 kbp。 HL-60中的染色体外分子显示在一个细胞周期内半保守复制,并且大约复制一次。我们建议这些亚显微元素是双倍染色体的前体,这是基因扩增的通常染色体外表现,因为两者在结构上相似并且可以自动复制。

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