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Somatic mutation in PIK3CA is a late event in cervical carcinogenesis

机译:PIK3CA的体细胞突变是宫颈癌发生的晚期事件

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AbstractSomatic mutations in cervical intraepithelial neoplasia (CIN) are largely unknown. Here, we profiled 35 cervical carcinomas and 23 CIN grade 2/3 (CIN2/3) for mutations in 48 cancer-related genes using a Next Generation Sequencing-based cancer panel. PIK3CA exon 9 was the most frequently mutated locus in cervical carcinoma and the only mutated locus detected in CIN2/3. These PIK3CA exon 9 mutation findings were verified in a large, independent series (n = 647) covering all stages of cervical carcinogenesis using high resolution melting-guided Sanger sequencing. PIK3CA exon 9 mutation frequency was 37.1% (13/35; 95%CI 21.2–54.0%) in cervical carcinoma, and 2.4% (5/209; 95%CI 0.5–4.7%) in CIN3. No PIK3CA exon 9 mutations were detected in CIN2 (0/144), CIN1 (0/154) and normal cervix (0/105). In a third series of 46 CIN2/3 lesions from women with a known 5-year history of preceding high-risk human papillomavirus (hrHPV) infection, detection of PIK3CA exon 9 mutation was confined to 2 (5.4%; 95%CI 0.0–13.2%) CIN3 lesions with preceding hrHPV infection ≥5 years, and was absent in those with a short duration (5 years) of preceding hrHPV infection. In conclusion, somatic mutation in PIK3CA represents a late event during cervical carcinogenesis, detected in a substantial subset of cervical carcinoma, but only in a minority of CIN3.
机译:摘要宫颈上皮内瘤变(CIN)的体细胞突变在很大程度上尚不清楚。在这里,我们使用了基于下一代测序的癌症专家组,分析了35种宫颈癌和23种CIN 2/3(CIN2 / 3)在48种与癌症相关的基因中的突变。 PIK3CA外显子9是宫颈癌中最常见的突变基因座,也是CIN2 / 3中唯一检测到的突变基因座。这些PIK3CA外显子9突变的发现已使用高分辨率熔解引导Sanger测序法在一个大的独立系列(n = 647)中进行了验证,涵盖宫颈癌的各个阶段。在宫颈癌中,PIK3CA外显子9突变的频率为37.1%(13/35; 95%CI 21.2–54.0%),在CIN3中为2.4%(5/209; 95%CI 0.5–4.7%)。在CIN2(0/144),CIN1(0/154)和正常子宫颈(0/105)中未检测到PIK3CA外显子9突变。在先前有高危人类乳头瘤病毒(hrHPV)感染已有5年历史的女性中,第三组46个CIN2 / 3病变中,PIK3CA外显子9突变的检测仅限于2个(5.4%; 95%CI 0.0– 13.2%)先前hrHPV感染≥5年的CIN3病变,而在先前hrHPV感染持续时间短(<5年)的患者中不存在。总之,PIK3CA中的体细胞突变代表宫颈癌发生过程中的晚期事件,在大部分子宫颈癌中检出,但仅在少数CIN3中检出。

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