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Chromosomal breakage-fusion-bridge events cause genetic intratumor heterogeneity

机译:染色体断裂-融合-桥事件导致遗传内肿瘤异质性

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It has long been known that rearrangements of chromosomes through breakage-fusion-bridge (BFB) cycles may cause variability of phenotypic and genetic traits within a cell population. Because intercellular heterogeneity is often found in neoplastic tissues, we investigated the occurrence of BFB events in human solid tumors. Evidence of frequent BFB events was found in malignancies that showed unspecific chromosome aberrations, including ring chro- mosomes, dicentric chromosomes, and telomeric associations, as well as extensive intratumor heterogeneity in the pattern of structural changes but not in tumors with tumor-specific aberra- tions and low variability. Fluorescence in situ hybridization analysis demonstrated that chromosomes participating in anaphase bridge formation were involved in a significantly higher number of structural aberrations than other chromosomes. Tumors with BFB events showed a decreased elimination rate of unstable chromo- some aberrations after irradiation compared with normal cells and other tumor cells. This result suggests that a combination of mitotically unstable chromosomes and an elevated tolerance to chromosomal damage leads to constant genomic reorganization in many malignancies, thereby providing a flexible genetic system for clonal evolution and progression.
机译:早已知道,通过断裂-融合-桥(BFB)循环进行的染色体重排可能会导致细胞群体内表型和遗传性状的变异。由于通常在肿瘤组织中发现细胞间异质性,因此我们研究了人实体瘤中BFB事件的发生。在恶性肿瘤中发现了频繁发生的BFB事件的证据,这些恶性肿瘤表现出非特异性的染色体畸变,包括环染色体,双着丝粒染色体和端粒缔合,以及结构改变模式中的广泛肿瘤内异质性,而在具有肿瘤特异性畸形的肿瘤中则没有。位置和低变异性。荧光原位杂交分析表明,参与后期桥形成的染色体比其他染色体参与的结构像差明显更高。与正常细胞和其他肿瘤细胞相比,具有BFB事件的肿瘤在放射后显示出不稳定的染色体异常消除率降低。该结果表明,有丝分裂不稳定的染色体和对染色体损伤的提高的耐受性的组合导致许多恶性肿瘤中恒定的基因组重组,从而为克隆的进化和进展提供了灵活的遗传系统。

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