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HRAS mutations in bladder cancer at an early age and the possible association with the Costello Syndrome

机译:早期膀胱癌中的HRAS突变及其可能与Costello综合征相关

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Bladder tumours of patients and20 years have a low incidence of genetic aberrations typically found in tumours in older patients. In this study, we investigated oncogene mutations in patients with bladder cancer (BC) and20 years and compared them to older age groups. Interestingly, we observed a relatively high number of HRAS mutations in tumour from young patients. These mutations were also highly uncommon in BCs of older patients, ie, p.(Gly12Ser) and p.(Gly12Ala). Germline mutations in the HRAS gene, especially p.(Gly12Ser/Ala), cause Costello Syndrome (CS), a severe congenital disorder. Indeed, one of the patients had been diagnosed with CS. We hypothesized that some of the other patients might be mosaic for the HRAS mutation and therefore could express some of the clinical features of CS, like tumour predisposition. Hence, we isolated DNA from microdissected stroma and analysed it for HRAS mutations. In the CS patient and in patient X, the mutation was also highly expressed in normal stroma. We conclude that patient X is possibly mosaic for the HRAS mutation. These results suggest that mosaicism for oncogenic HRAS mutations may increase the risk for developing BC at a young age.
机译:患者和20岁以下的膀胱肿瘤的遗传畸变发生率较低,通常在老年患者的肿瘤中发现。在这项研究中,我们调查了20岁及以下的膀胱癌(BC)患者的癌基因突变,并将其与年龄较大的人群进行了比较。有趣的是,我们在年轻患者的肿瘤中观察到相对大量的HRAS突变。这些突变在老年患者的BC中也很罕见,即p。(Gly12Ser)和p。(Gly12Ala)。 HRAS基因中的种系突变,特别是p。(Gly12Ser / Ala)引起严重的先天性疾病科斯特洛综合症(CS)。实际上,其中一名患者被诊断出患有CS。我们假设其他一些患者可能是HRAS突变的镶嵌体,因此可以表达CS的某些临床特征,例如肿瘤易感性。因此,我们从显微解剖的基质中分离了DNA,并对其进行了HRAS突变分析。在CS患者和X患者中,该突变也在正常基质中高表达。我们得出结论,患者X可能是HRAS突变的镶嵌体。这些结果表明,致癌性HRAS突变的镶嵌术可能会增加年轻时发生BC的风险。

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