首页> 外文期刊>The Journal of molecular diagnostics: JMD >Nine novel germline gene variants in the RET proto-oncogene identified in twelve unrelated cases.
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Nine novel germline gene variants in the RET proto-oncogene identified in twelve unrelated cases.

机译:在十二个无关病例中鉴定出RET原癌基因中的九个新种系基因变体。

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摘要

We report nine novel DNA alterations in the RET proto-oncogene in 12 unrelated cases identified by DNA sequencing of exons 10 and 11 of the gene. The novel variants K666E, IVS9-11G-->A, D631V in cis with H665Q, D631E (with C634Y), E623K (in trans with C618S), 616delGAG (in trans with C609Y), Y606C, C630R, and R635-T636insELCR;T636P were detected in patients with various clinical presentations ranging from thyroid goiter, medullary thyroid carcinoma, and pheochromocytoma to classic multiple endocrine neoplasia type 2A. When novel DNA alterations are found, extended family studies can be helpful in determining the clinical significance of such findings. Segregation within families suggests that K666E and T636insELCR;T636P are likely to be disease-causing mutations. However, the mechanism by which they affect the normal activity of the RET receptor is unclear. Absence of segregation with disease was observed for E623K and 616delGAG. For the remainder of the DNA alterations, family studies were not possible, and the clinical significance of these novel variants needs further assessment. Additional case reports, animal models, and/or functional studies are needed to determine the clinical significance of these newly identified variants.
机译:我们报告了通过基因外显子10和11的DNA测序鉴定的12个无关病例中RET原癌基因中的9种新颖的DNA改变。新的变体K666E,IVS9-11G-> A,D631V与H665Q顺式,D631E(与C634Y结合),E623K(与C618S结合),616delGAG(与C609Y结合),Y606C,C630R和R635-T636insELCR从甲状腺肿大,甲状腺髓样癌和嗜铬细胞瘤到典型的多发性内分泌肿瘤2A型,临床表现各异的患者中检测到T636P。当发现新的DNA改变时,大家庭研究可能有助于确定此类发现的临床意义。家庭内部的隔离表明,K666E和T636insELCR; T636P可能是致病突变。然而,它们影响RET受体正常活性的机制尚不清楚。对于E623K和616delGAG,观察到没有疾病隔离。对于其余的DNA改变,不可能进行家族研究,并且这些新变体的临床意义需要进一步评估。需要其他病例报告,动物模型和/或功能研究来确定这些新发现的变体的临床意义。

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