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BRAF copy number gains in thyroid tumors detected by fluorescence In Situ hybridization

机译:通过荧光原位杂交检测甲状腺肿瘤中的BRAF拷贝数增加

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摘要

Point mutation of the BRAF gene is a common genetic event in papillary thyroid carcinomas. More recently, it has been found that BRAF can also participate in chromosomal rearrangement. In this study, we explore yet another possible mechanism of BRAF alteration, which involves copy number gain. Using fluorescence in situ hybridization with BRAF specific and chromosome 7 centromeric probes, we studied 62 follicular thyroid tumors and 32 papillary carcinomas. We found that numerical changes in BRAF copy number were rare in papillary thyroid carcinomas, while they occurred in 16–45% of follicular tumors of conventional and oncocytic (Hürthle cell) types. They were due to amplification of the gene or gain of one or more copies of chromosome 7. Tetrasomy for chromosome 7 was overall the most common finding. The changes in BRAF copy number did not overlap with RAS mutations in follicular tumors. In a group of follicular carcinomas, tumors with BRAF copy number gain were significantly more often widely invasive (67%) compared to tumors with no copy number change (18%). By Western blotting, the tumors carrying four copies of the gene revealed higher expression of BRAF protein, suggesting that copy number gain may represent another mechanism of BRAF activation in thyroid tumors.
机译:在甲状腺乳头状癌中,BRAF基因的点突变是常见的遗传事件。最近,已经发现BRAF也可以参与染色体重排。在这项研究中,我们探索了BRAF改变的另一种可能机制,该机制涉及拷贝数增加。使用BRAF特异性和染色体7着丝粒探针荧光原位杂交,我们研究了62例滤泡性甲状腺肿瘤和32例乳头状癌。我们发现,BRAF拷贝数的数值变化在甲状腺乳头状癌中很少见,而在传统型和吞噬性(Hürthle细胞)类型的滤泡性肿瘤中则发生于16%至45%。它们是由于基因的扩增或获得7号染色体的一个或多个副本而引起的。对7号染色体的四染色体切开术总体上是最常见的发现。在滤泡性肿瘤中,BRAF拷贝数的变化与RAS突变不重叠。在一组滤泡癌中,与无拷贝数变化的肿瘤(18%)相比,具有BRAF拷贝数增加的肿瘤更常被广泛浸润(67%)。通过蛋白质印迹法,携带该基因的四个拷贝的肿瘤显示出BRAF蛋白的更高表达,这表明拷贝数的增加可能代表了甲状腺肿瘤中BRAF活化的另一种机制。

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