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首页> 外文期刊>Nature Communications >Cell–cell adhesion genes CTNNA2 and CTNNA3 are tumour suppressors frequently mutated in laryngeal carcinomas
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Cell–cell adhesion genes CTNNA2 and CTNNA3 are tumour suppressors frequently mutated in laryngeal carcinomas

机译:细胞间粘附基因 CTNNA2 CTNNA3 是在体内经常发生突变的抑癌基因喉癌

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Laryngeal squamous cell carcinoma is a frequent and significant cause of morbidity and mortality. Here we explore the biological basis of this aggressive tumour, and identify two cell–cell adhesion genes as recurrently mutated in this malignancy. We first perform exome sequencing of four laryngeal carcinomas and their matched normal tissues. Among the 569 genes found to present somatic mutations, and based on their recurrence or functional relevance in cancer, we select 40 for further validation in 86 additional laryngeal carcinomas. We detect frequent mutations (14 of 90, 15%) in CTNNA2 and CTNNA3 -encoding α-catenins. Functional studies reveal an increase in the migration and invasive ability of head and neck squamous cell carcinoma cells producing mutated forms of CTNNA2 and CTNNA3 or in cells where both α-catenins are silenced. Analysis of the clinical relevance of these mutations demonstrates that they are associated with poor prognosis. We conclude that CTNNA2 and CTNNA3 are tumour suppressor genes frequently mutated in laryngeal carcinomas.
机译:喉鳞状细胞癌是发病和死亡的常见原因。在这里,我们探讨了这种侵袭性肿瘤的生物学基础,并确定了在这种恶性肿瘤中反复突变的两个细胞间粘附基因。我们首先对四种喉癌及其匹配的正常组织进行外显子组测序。在发现存在体细胞突变的569个基因中,根据它们在癌症中的复发或功能相关性,我们选择40个基因进一步在86个其他喉癌中进行验证。我们在CTNNA2和CTNNA3编码α-catenins中检测到频繁的突变(90个中的14个,占15%)。功能研究表明,产生突变形式的CTNNA2和CTNNA3的头颈部鳞状细胞癌细胞或两种α-catenins都沉默的细胞的迁移和侵袭能力增加。对这些突变的临床相关性分析表明,它们与不良预后有关。我们得出的结论是CTNNA2和CTNNA3是在喉癌中经常突变的抑癌基因。

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