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首页> 外文期刊>Familial Cancer >Non-truncating hMLH1 variants identified in Slovenian gastric cancer patients are not associated with Lynch Syndrome: a functional analysis report
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Non-truncating hMLH1 variants identified in Slovenian gastric cancer patients are not associated with Lynch Syndrome: a functional analysis report

机译:斯洛文尼亚胃癌患者中发现的非截断型hMLH1变异与Lynch综合征无关:功能分析报告

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摘要

Hereditary non-polyposis colorectal cancer is the most common known genetic syndrome that predisposes to various types of cancer including gastric cancer and occures mainly due to pathogenic germline mutations in DNA mismatch repair (MMR) genes, such as MLH1, MSH2 and MSH6. Impaired MMR activity can lead to microsatellite instability (MSI) in tumor tissues. Interpreting the pathogenic significance of identified mutations in MMR genes, especially missense alterations and short in-frame deletions and insertions is challenging and functional analysis is often needed to accurately assess their pathogenicities. The purpose of this study was to evaluate functional significance of MLH1 missense mutations, previously identified in unrelated Slovenian patients with MSI-positive gastric carinomas. A novel in vivo yeast-based approach and in silico predictions were used. Variant E433Q was characterized for the first time and was shown to have no effect on MLH1 protein function. Functional analysis of amino acid rearrangement K618A, with previously reported contradictory results of its pathogenicity, suggests that the variant is a neutral polymorphism. Results of our study imply that there is either germline mutation or an epigenetic inactivation of another MMR gene, which causes MSI phenotype in the referred gastric cancer cases.
机译:遗传性非息肉病性结直肠癌是最常见的遗传综合征,易患各种类型的癌症,包括胃癌,其发生主要是由于DNA错配修复(MMR)基因中的病原种系突变,例如MLH1,MSH2和MSH6。 MMR活性受损可导致肿瘤组织中的微卫星不稳定性(MSI)。解释MMR基因中已鉴定突变的致病意义,尤其是错义变异和短框内缺失和插入,具有挑战性,通常需要进行功能分析以准确评估其致病性。这项研究的目的是评估MLH1错义突变的功能意义,该突变先前已在不相关的斯洛文尼亚MSI阳性胃癌患者中发现。使用了一种新颖的基于体内酵母的方法和计算机模拟预测。变体E433Q首次进行了表征,显示对MLH1蛋白功能没有影响。氨基酸重排K618A的功能分析,与先前报道的其致病性矛盾的结果表明,该变体是中性多态性。我们的研究结果表明,存在另一种MMR基因的种系突变或表观遗传失活,这在所提及的胃癌病例中会导致MSI表型。

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