Frequent loss of the AXIN1 locus but absence of AXIN1 gene mutations in adenocarcinomas of the gastro-oesophageal junction with nuclear |[beta]|-catenin expression

L B Koppert; A W van der Velden; M van de Wetering; M Abbou; A M W van den Ouweland; H W Tilanus; B P L Wijnhoven; W N M Dinjens

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Frequent loss of the AXIN1 locus but absence of AXIN1 gene mutations in adenocarcinomas of the gastro-oesophageal junction with nuclear |[beta]|-catenin expression

机译：具有核|β|-连环蛋白表达的胃食管交界处腺癌中AXIN1基因座的频繁丢失但AXIN1基因突变不存在

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Up to 60% of gastro-oesophageal junction (GEJ) adenocarcinomas show nuclear β-catenin expression, pointing to activated T-cell factor (TCF)/β-catenin-driven gene transcription. We demonstrate in five human GEJ adenocarcinoma cell lines that nuclear β-catenin expression indeed correlates with enhanced TCF-mediated transcription of a reporter gene. In several tumour types, TCF/β-catenin activation is caused by mutations in either adenomatous polyposis coli (APC), β-catenin exon 3, AXIN1, AXIN2 or β-transducin repeat-containing protein (β-TrCP). In GEJ adenocarcinomas, very few APC and β-catenin mutations have been found. Therefore, the mechanism of Wnt pathway activation remains unclear. In the present study, we did not find AXIN1 gene mutations in 17 GEJ tumours with nuclear β-catenin expression (without β-catenin exon 3 mutations). Six intragenic single nucleotide polymorphisms (SNPs) were identified. One of these, the AXIN1 gene T1942C SNP, has a frequency of 21% but is only very recently described despite numerous AXIN1 gene mutational studies. We provide evidence why this SNP was missed in single strand conformation polymorphism analyses. The AXIN1 gene G2063A variation was previously described as a gene mutation but we demonstrate that this is a polymorphism. With these six SNPs loss of heterozygosity (LOH) was found in 11 of 15 (73%) informative tumours. To investigate a possible AXIN1 gene dosage effect in GEJ tumours expressing nuclear β-catenin, AXIN1 locus LOH was determined in 20 tumours expressing membranous and no nuclear β-catenin. LOH was found in 10 of 13 (77%) informative cases. AXIN1 protein immunohistochemistry revealed cytoplasmic expression in all tumours irrespective of the presence of AXIN1 locus LOH. These data indicate that nuclear β-catenin expression is indicative for activated Wnt signalling and that neither AXIN1 gene mutations nor AXIN1 locus LOH are involved in Wnt pathway activation in GEJ adenocarcinomas.

机译：高达60％的胃食管连接（GEJ）腺癌显示核β-catenin表达，表明活化的T细胞因子（TCF）/β-catenin驱动的基因转录。我们在五个人类GEJ腺癌细胞系中证明，核β-连环蛋白的表达确实与增强的TCF介导的报道基因转录相关。在几种肿瘤类型中，TCF /β-catenin激活是由腺瘤性息肉病（APC），β-catenin外显子3，AXIN1，AXIN2或包含β-转导蛋白重复蛋白（β-TrCP）的突变引起的。在GEJ腺癌中，很少发现APC和β-catenin突变。因此，Wnt途径激活的机制仍不清楚。在本研究中，我们没有在17个具有核β-catenin表达的GEJ肿瘤中发现AXIN1基因突变（无β-catenin外显子3突变）。确定了六个基因内单核苷酸多态性（SNP）。其中之一，AXIN1基因T1942C SNP的频率为21％，但尽管有许多AXIN1基因突变研究，但直到最近才被描述。我们提供证据，为什么在单链构象多态性分析中错过了此SNP。 AXIN1基因G2063A变异以前被描述为基因突变，但我们证明这是一个多态性。在这16个SNP中，有15个中的11个（73％）发生了杂合性（LOH）丢失（73％）。为了研究在表达核β-catenin的GEJ肿瘤中可能的AXIN1基因剂量效应，在20种表达膜性且无核β-catenin的肿瘤中确定了AXIN1基因座LOH。在13例信息丰富的案例中，有10例发现了LOH（77％）。 AXIN1蛋白免疫组化显示，在所有肿瘤中均存在胞质表达，而与AXIN1基因座LOH无关。这些数据表明核β-catenin表达指示激活的Wnt信号，并且AXIN1基因突变和AXIN1基因座LOH均不参与GEJ腺癌的Wnt途径激活。

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《British Journal of Cancer》 |2004年第4期|共8页
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L B Koppert; A W van der Velden; M van de Wetering; M Abbou; A M W van den Ouweland; H W Tilanus; B P L Wijnhoven; W N M Dinjens;
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6. Frequent loss of the AXIN1 locus but absence of AXIN1 gene mutations in adenocarcinomas of the gastro-oesophageal junction with nuclear β-catenin expression [O] . L B Koppert, A W van der Velden, M van de Wetering, 2004

机译：带有核β-catenin表达的胃食管交界处腺癌中AXIN1基因座的频繁丢失但AXIN1基因突变不存在
7. Frequent loss of the AXIN1 locus but absence of AXIN1 gene mutations in adenocarcinomas of the gastro-oesophageal junction with nuclear β-catenin expression [O] . Koppert, L.B. (Linetta), Velden, A.W. (Albertina) van der, Wetering, M. (M.) van de, 2004

机译：带有核β-catenin表达的胃食管交界处腺癌中AXIN1基因座的频繁丢失但AXIN1基因突变不存在

Frequent loss of the AXIN1 locus but absence of AXIN1 gene mutations in adenocarcinomas of the gastro-oesophageal junction with nuclear |[beta]|-catenin expression

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