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年轻胃癌先证者中与E-钙黏蛋白功能失活相关的CDH1种系错义突变的鉴定

Identification of CDH1 germline missense mutations associated with functional inactivation of the E-cadherin protein in young gastric cancer probands.

作者信息

Suriano Gianpaolo, Oliveira Carla, Ferreira Paulo, Machado José C, Bordin Maria C, De Wever Olivier, Bruyneel Erik A, Moguilevsky Nicole, Grehan Nicola, Porter Timothy R, Richards Frances M, Hruban Ralph H, Roviello Franco, Huntsman David, Mareel Marc, Carneiro Fátima, Caldas Carlos, Seruca Raquel

机构信息

Instituto de Patologia e Imunologia Molecular da Universidade do Porto, 4200 Porto, Portugal.

出版信息

Hum Mol Genet. 2003 Mar 1;12(5):575-82. doi: 10.1093/hmg/ddg048.

Abstract

E-cadherin is involved in the formation of cell-junctions and the maintenance of epithelial integrity. Direct evidence of E-cadherin mutations triggering tumorigenesis has come from the finding of inactivating germline mutations of the gene (CDH1) in hereditary diffuse gastric cancer (HDGC). We screened a series of 66 young gastric cancer probands for germline CDH1 mutations, and two novel missense alterations together with an intronic variant were identified. We then analysed the functional significance of the two exonic missense variants found here as well as a third germline missense variant that we previously identified in a HGDC family. cDNAs encoding either the wild-type protein or mutant forms of E-cadherin were stably transfected into CHO (Chinese hamster ovary) E-cadherin-negative cells. Transfected cell-lines were characterized in terms of aggregation, motility and invasion. We show that a proportion of apparently sporadic early-onset diffuse gastric carcinomas are associated with germline alterations of the E-cadherin gene. We also demonstrate that a proportion of missense variants are associated with significant functional consequences, suggesting that our cell model can be used as an adjunct in deciding on the potential pathogenic role of identified E-cadherin germline alterations.

摘要

E-钙黏蛋白参与细胞连接的形成以及上皮完整性的维持。E-钙黏蛋白突变引发肿瘤发生的直接证据来自于遗传性弥漫性胃癌(HDGC)中该基因(CDH1)种系失活突变的发现。我们对66例年轻胃癌先证者进行了种系CDH1突变筛查,鉴定出两个新的错义改变以及一个内含子变异。然后,我们分析了此处发现的两个外显子错义变异以及我们先前在一个HGDC家族中鉴定出的第三个种系错义变异的功能意义。将编码野生型蛋白或E-钙黏蛋白突变形式的cDNA稳定转染至CHO(中国仓鼠卵巢)E-钙黏蛋白阴性细胞中。对转染细胞系的聚集、运动和侵袭情况进行了表征。我们发现,一部分明显散发的早发性弥漫性胃癌与E-钙黏蛋白基因的种系改变有关。我们还证明,一部分错义变异与显著的功能后果相关,这表明我们的细胞模型可作为辅助手段,用于确定已鉴定的E-钙黏蛋白种系改变的潜在致病作用。

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