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遗传性弥漫性胃癌家族中的新型种系CDH1突变

Novel germline CDH1 mutations in hereditary diffuse gastric cancer families.

作者信息

Humar Bostjan, Toro Tumi, Graziano Francesco, Müller Hansjakob, Dobbie Zuzana, Kwang-Yang Han, Eng Charis, Hampel Heather, Gilbert Dale, Winship Ingrid, Parry Susan, Ward Robyn, Findlay Mike, Christian Alice, Tucker Monica, Tucker Kathy, Merriman Tony, Guilford Parry

机构信息

Cancer Genetics Laboratory, Department of Biochemistry, University of Otago, Dunedin, New Zealand.

出版信息

Hum Mutat. 2002 May;19(5):518-25. doi: 10.1002/humu.10067.

Abstract

Hereditary diffuse gastric cancer (HDGC) is a recently defined cancer syndrome caused by inactivating, heterozygous germline mutations in the gene for the cell-to-cell adhesion protein E-cadherin (CDH1). Here, we describe the search for CDH1 mutations in 10 newly identified gastric cancer families. Seven of 10 families met the clinical criteria for HDGC. Germline mutations were identified in four of these seven families and one family that was borderline for the clinical criteria. Of the mutations identified in the five new families, four were previously unreported and consisted of two frameshift and two donor splice site mutations. One splice site mutation occurred at the 100% conserved +1 position. The second splice site mutation occurred at the +5 position and was shown to lead to abnormal splicing. Additional CDH1 variants detected include the heterozygous -160 C-->A promoter polymorphism, which has previously been reported to be associated with decreased CDH1 transcription. We, however, found this polymorphism to be common in a control population, suggesting that a major role for this polymorphism in gastric cancer susceptibility is unlikely.

摘要

遗传性弥漫性胃癌(HDGC)是一种最近定义的癌症综合征,由细胞间粘附蛋白E-钙粘蛋白(CDH1)基因的失活杂合种系突变引起。在此,我们描述了在10个新发现的胃癌家族中寻找CDH1突变的过程。10个家族中有7个符合HDGC的临床标准。在这7个家族中的4个以及1个临床标准处于临界状态的家族中发现了种系突变。在这5个新家族中鉴定出的突变中,有4个是以前未报告过的,包括2个移码突变和2个供体剪接位点突变。一个剪接位点突变发生在100%保守的+1位置。第二个剪接位点突变发生在+5位置,并被证明会导致异常剪接。检测到的其他CDH1变体包括杂合的-160 C→A启动子多态性,此前有报道称该多态性与CDH1转录减少有关。然而,我们发现这种多态性在对照人群中很常见,这表明该多态性在胃癌易感性中不太可能起主要作用。

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