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胃癌中复制错误改变位点及微卫星不稳定性相关突变的临床病理意义

Clinicopathological significance of altered loci of replication error and microsatellite instability-associated mutations in gastric cancer.

作者信息

Wu M S, Lee C W, Shun C T, Wang H P, Lee W J, Sheu J C, Lin J T

机构信息

Department of Internal Medicine, National Taiwan University Hospital, Taipei, Republic of China.

出版信息

Cancer Res. 1998 Apr 1;58(7):1494-7.

PMID:9537253
Abstract

Replication errors (RERs) judged by microsatellite instability and its associated mutations have been recognized as an important mechanism in tumorigenesis of gastric cancers (GCs). To gain a deeper insight into its significance, we examined the frequency of RERs using nine microsatellite markers and screened mutations in the polydeoxyadenine tract of the transforming growth factor beta type II receptor gene (TGF-betaRII) and polydeoxyguanine tracts of insulin-like growth factor II receptor and BAX genes. Twenty-four (30%) of 80 patients with GC had RERs, of which 3, 8, and 13 had one, two, and three or more loci, respectively. In 13 tumors with RERs in three or more loci, frameshift mutations of TGF-betaRII, insulin-like growth factor II receptor, and BAX were identified in 12, 3, and 2, respectively. Compared with GC with none, one or two RER-positive loci as a group, GC with RERs in three or more loci showed a significantly higher frequency of antral location (12 of 13 versus 35 of 67; P = 0.01), intestinal subtype (11 of 13 versus 30 of 67; P = 0.01), and previous Helicobacter pylori infection (12 of 13 versus 41 of 67; P = 0.05) and a lower incidence of lymph node metastasis (5 of 13 versus 49 of 67; P = 0.02) and tended to be in an advanced stage (12 of 13 versus 54 of 67; P = 0.28). These data indicate that GC with multiple RERs manifest distinct clinicopathological characteristics, and that a high frequency of frameshift mutations involving the TGF-betaRII gene may be causatively linked with tumorigenesis and progression.

摘要

通过微卫星不稳定性及其相关突变判断的复制错误(RERs)已被认为是胃癌(GCs)肿瘤发生的重要机制。为了更深入了解其意义,我们使用9个微卫星标记检查了RERs的频率,并筛选了转化生长因子βII型受体基因(TGF-βRII)的多聚脱氧腺嘌呤序列以及胰岛素样生长因子II受体和BAX基因的多聚脱氧鸟嘌呤序列中的突变。80例GC患者中有24例(30%)存在RERs,其中3例、8例和13例分别有1个、2个和3个或更多位点。在13个有3个或更多位点RERs的肿瘤中,分别在12个、3个和2个肿瘤中鉴定出TGF-βRII、胰岛素样生长因子II受体和BAX的移码突变。与无RERs、1个或2个RER阳性位点的GC作为一组相比,有3个或更多位点RERs的GC显示胃窦部位置频率显著更高(13例中的12例对67例中的35例;P = 0.01)、肠型(13例中的11例对67例中的30例;P = 0.01)以及既往幽门螺杆菌感染率更高(13例中的12例对67例中的41例;P = 0.05),且淋巴结转移发生率更低(13例中的5例对67例中的49例;P = 0.02),并且倾向于处于晚期(13例中的12例对67例中的54例;P = 0.28)。这些数据表明,具有多个RERs的GC表现出明显的临床病理特征,并且涉及TGF-βRII基因的高频移码突变可能与肿瘤发生和进展有因果关系。

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