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The Role of Dicentric Chromosome Formation and Secondary Centromere Deletion in the Evolution of Myeloid Malignancy

机译:双着丝粒染色体形成和次级着丝粒删除在髓系恶性肿瘤演变中的作用。

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摘要

Dicentric chromosomes have been identified as instigators of the genome instability associated with cancer, but this instability is often resolved by one of a number of different secondary events. These include centromere inactivation, inversion, and intercentromeric deletion. Deletion or excision of one of the centromeres may be a significant occurrence in myeloid malignancy and other malignancies but has not previously been widely recognized, and our reports are the first describing centromere deletion in cancer cells. We review what is known about dicentric chromosomes and the mechanisms by which they can undergo stabilization in both constitutional and cancer genomes. The failure to identify centromere deletion in cancer cells until recently can be partly explained by the standard approaches to routine diagnostic cancer genome analysis, which do not identify centromeres in the context of chromosome organization. This hitherto hidden group of primary dicentric, secondary monocentric chromosomes, together with other unrecognized dicentric chromosomes, points to a greater role for dicentric chromosomes in cancer initiation and progression than is generally acknowledged. We present a model that predicts and explains a significant role for dicentric chromosomes in the formation of unbalanced translocations in malignancy.
机译:双中心染色体已被确定为与癌症相关的基因组不稳定性的诱因,但是这种不稳定性通常可以通过许多不同的继发性事件之一来解决。这些包括着丝粒失活,倒位和着丝粒间缺失。在髓样恶性肿瘤和其他恶性肿瘤中,着丝粒之一的缺失或切除可能是一个重要事件,但以前尚未得到广泛认可,我们的报道是第一个描述癌细胞中着丝粒缺失的研究。我们回顾了有关双着丝粒染色体的知识以及它们在体质和癌症基因组中可以稳定的机制。直到最近才未能确定癌细胞中着丝粒缺失,这可以通过常规诊断性癌症基因组分析的标准方法来部分解释,该标准方法不能在染色体组织的背景下识别着丝粒。迄今为止,这一隐藏的初级双中心,次级单中心染色体组以及其他无法识别的双中心染色体表明,双中心染色体在癌症发生和发展中的作用要比公认的更大。我们提出了一个模型,该模型预测并解释了双中心染色体在恶性肿瘤中不平衡易位形成中的重要作用。

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