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Delineating Chromosomal Breakpoints in Radiation-Induced Papillary Thyroid Cancer

机译:描绘辐射诱发的乳头状甲状腺癌的染色体断裂点

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摘要

Recurrent translocations are well known hallmarks of many human solid tumors and hematological disorders, where patient- and breakpoint-specific information may facilitate prognostication and individualized therapy. In thyroid carcinomas, the proto-oncogenes RET and NTRK1 are often found to be activated through chromosomal rearrangements. However, many sporadic tumors and papillary thyroid carcinomas (PTCs) arising in patients with a history of exposure to elevated levels of ionizing irradiation do not carry these known abnormalities. We developed a rapid scheme to screen tumor cell metaphase spreads and identify candidate genes of tumorigenesis and neoplastic progression for subsequent functional studies. Using a series of overnight fluorescence in situ hybridization (FISH) experiments with pools comprised of bacterial artificial chromosome (BAC) clones, it now becomes possible to rapidly refine breakpoint maps and, within one week, progress from the low resolution Spectral Karyotyping (SKY) maps or Giemsa-banding (G-banding) karyotypes to fully integrated, high resolution physical maps including a list of candiate genes in the critical regions.
机译:反复易位是许多人类实体瘤和血液系统疾病的众所周知的特征,其中患者和断点的特定信息可能有助于预后和个体化治疗。在甲状腺癌中,经常发现原癌基因RET和NTRK1通过染色体重排被激活。但是,在有高水平电离辐射暴露史的患者中出现的许多散发性肿瘤和甲状腺乳头状癌(PTC)并未携带这些已知异常。我们开发了一种快速的方案,以筛选肿瘤细胞中期扩散,并确定肿瘤发生和肿瘤进展的候选基因,用于后续功能研究。使用一系列夜间荧光原位杂交(FISH)实验,对包含细菌人工染色体(BAC)克隆的库进行分析,现在可以快速完善断点图,并在一周之内从低分辨率光谱核型分析(SKY)取得进展图或Giemsa谱带(G谱带)核型到完全整合的高分辨率物理图谱,包括关键区域的候选基因列表。

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