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Increased BRAF copy number in lung adenocarcinoma

机译:肺腺癌中BRAF拷贝数增加

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Point mutation of the BRAF gene is a genetic event that occurs in a subset of lung adenocarcinoma cases. For example, BRAF V600E is a driver mutation that can be effectively targeted using selective BRAF and/or MEK inhibitors. The present study hypothesized that an increase in BRAF copy number may be correlated with certain clinicopathological features of lung adenocarcinoma in Japanese patients. The BRAF gene copy number was analyzed using quantitative polymerase chain reaction amplifications in 29 surgically treated lung adenocarcinoma cases without EGFR or Kras mutations from Nagoya City University Hospital (Nagoya, Japan). Seven BRAF-mutant cases were included. Increased BRAF gene copy number was identified in three lung adenocarcinoma patients (10.3%), all of which exhibited the V600E mutation. Using fluorescence in situ hybridization with BRAF-specific and chromosome 7 centromeric probes, increased copy number status was associated with gene amplification or gain of chromosome 7. Although increased BRAF copy number was correlated with BRAF V600E mutations, numerical changes in BRAF copy number were rare and mild in lung adenocarcinoma, resulting in no significant difference in pathological tumor status or tumor stage.
机译:BRAF基因的点突变是遗传事件,发生在一部分肺腺癌病例中。例如,BRAF V600E是可以使用选择性BRAF和/或MEK抑制剂有效靶向的驱动程序突变。本研究假设,BRAF拷贝数的增加可能与日本患者肺腺癌的某些临床病理特征有关。使用来自名古屋市大学医院(日本名古屋)的29例无EGFR或Kras突变的经手术治疗的肺腺癌病例,通过定量聚合酶链反应扩增分析了BRAF基因的拷贝数。包括7例BRAF突变病例。在三名肺腺癌患者(10.3%)中发现BRAF基因拷贝数增加,所有患者均表现出V600E突变。使用BRAF特异性和7号染色体着丝粒探针进行荧光原位杂交,增加的拷贝数状态与基因扩增或7号染色体的获得有关。尽管增加的BRAF拷贝数与BRAF V600E突变相关,但很少发生BRAF拷贝数的数字变化在肺腺癌中为轻度,在病理性肿瘤状态或肿瘤分期方面无明显差异。

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