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Topoisomerase IIalpha gene (TOP2A) amplification and deletion in cancer - more common than anticipated.

机译:拓扑异构酶IIalpha基因(TOP2A)在癌症中的扩增和缺失-比预期的更为普遍。

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In solid tumours the predominant genetic mechanism for oncogene activation is through amplification of genes. The HER-2 (also known as ErbB2/c-erbB2/HER-2eu) oncogene is the most frequently amplified oncogene in breast cancer and is also commonly amplified in other forms of cancer. The HER-2 amplicon also contains other biologically relevant genes with altered copy numbers, among these genes is the topoisomerase IIalpha (TOP2A). TOP2A gene is located adjacent to the HER-2 oncogene at the chromosome location 17q12-q21 and is either amplified or deleted, with equal frequency, in almost 90% of HER-2 amplified primary breast tumours. Recent data suggest that amplification and deletion of TOP2A may account for both sensitivity and resistance to topoII-inhibitor-chemotherapy, depending on the specific genetic defect at the TOP2A locus. In this issue of the Cytopathology, Bofin et al. present preliminary evidence for high prevalance of TOP2A amplification and deletion not only in the HER-2 amplified breast tumours, but also in the primary breast tumours without the HER-2 amplification. This finding together with the concept that TOP2A gene amplification and deletion seem to account for both relative chemosensitivity and resistance to topoII-inhibitor therapy further highlights the importance of screening for TOP2A gene copy number aberrations when topoII-inhibitors are considered either alone or in combination of other chemotherapeutic drugs for the treatment of cancer patients.
机译:在实体瘤中,致癌基因激活的主要遗传机制是通过基因扩增。 HER-2(也称为ErbB2 / c-erbB2 / HER-2 / neu)癌基因是乳腺癌中最常见的扩增癌基因,也通常在其他形式的癌症中扩增。 HER-2扩增子还包含其他生物学相关基因,其拷贝数已改变,其中这些基因是拓扑异构酶IIalpha(TOP2A)。 TOP2A基因在染色体位置17q12-q21处与HER-2癌基因相邻,并且在几乎90%的HER-2扩增原发性肿瘤中以相等的频率被扩增或缺失。最近的数据表明,TOP2A的扩增和缺失可能解释了对topoII抑制剂化学疗法的敏感性和耐药性,这取决于TOP2A基因座的具体遗传缺陷。在本期《细胞病理学》中,Bofin等人。目前的初步证据表明,不仅在HER-2扩增的乳腺肿瘤中,而且在没有HER-2扩增的原发性乳腺肿瘤中,TOP2A扩增和缺失的发生率很高。这一发现与TOP2A基因扩增和缺失似乎说明了相对化学敏感性和对topoII抑制剂治疗的抗性的概念进一步突显了当单独或组合考虑topoII抑制剂时筛选TOP2A基因拷贝数异常的重要性。其他用于治疗癌症患者的化疗药物。

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