Inactivation of both alleles of the DPC4/SMAD4 gene in advanced colorectal cancers: identification of seven novel somatic mutations in tumors from Japanese patients

Masaaki Koyama , Masahide Ito , Hisaki Nagai , Mitsuru Emi , Yuukichi Moriyama
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引用次数: 62

Abstract

Loss of heterozygosity (LOH) of loci on chromosome 18q occurs in a majority of colorectal cancers. The DPC4/SMAD4 gene, lying in close proximity to the DCC gene at 18q21.1, was recently identified as a candidate tumor suppressor for the genesis of pancreatic cancer as well as a predisposing gene for Juvenile Polyposis Syndrome (JPS). The gene product functions as a cytoplasmic mediator in the signaling pathway of transforming growth factor beta (TGF-β). To investigate the potential role of DPC4/SMAD4 gene in colorectal cancers, we examined 73 tumors of clinical stages II or III from Japanese patients, for LOH at 18q21 and also for subtle mutations anywhere within the coding region of DPC4/SMAD4. LOH was identified in 50 (78%) of the 64 tumors that were informative for polymorphic markers in the region. Somatic mutations were identified in seven of those tumors: two frameshift mutations, a 1-bp deletion (326 del T) in exon 8 and a 1-bp insertion (50–51 ins A) in exon 1; two nonsense mutations, Arg445Ter in exon 10 and Glu538Ter in exon 11; and three missense mutations, Asn129Lys in exon 2, Tyr95Asn in exon 2, and Asp355Glu in exon 8. Three of the seven mutations were observed in the mad homology 1 (MH1) domain encoded by exons 1 and 2. In all of the tumors carrying intragenic mutations of one allele, LOH analysis had shown that the other allele was missing. The results demonstrated that inactivation of both alleles of the DPC4/SMAD4 gene occurs in a substantial proportion of advanced colorectal cancers, and that the DPC4/SMAD4 gene probably exerts a tumor-suppressor effect for colorectal carcinogenesis that fulfills the criterion of the two-hit concept proposed by Knudson [A.G. Knudson, Hereditary cancer, oncogenes, and anti-oncogenes, Cancer Res. 45 (1985) 1437–1443.].

晚期结直肠癌DPC4/SMAD4基因两个等位基因失活:日本患者肿瘤中7个新的体细胞突变的鉴定
18q染色体杂合性缺失(LOH)发生在大多数结直肠癌中。DPC4/SMAD4基因位于DCC基因18q21.1附近,最近被确定为胰腺癌发生的候选肿瘤抑制基因,以及青少年息肉病综合征(JPS)的易感基因。该基因产物在转化生长因子β (TGF-β)信号通路中起细胞质介质的作用。为了研究DPC4/SMAD4基因在结直肠癌中的潜在作用,我们检测了73例临床II期或III期日本患者的肿瘤,检测18q21处的LOH以及DPC4/SMAD4编码区任何地方的细微突变。64个肿瘤中有50个(78%)被鉴定出LOH,这些肿瘤对该区域的多态性标记具有信息。其中7个肿瘤中发现体细胞突变:2个移码突变,8外显子1 bp缺失(326 del T)和1外显子1 bp插入(50-51 in a);2个无义突变,分别位于第10外显子Arg445Ter和第11外显子Glu538Ter;3个错义突变,分别是外显子2的Asn129Lys、外显子2的Tyr95Asn和外显子8的Asp355Glu。7个突变中有3个发生在由外显子1和2编码的MH1结构域。在所有携带一个等位基因基因内突变的肿瘤中,LOH分析显示另一个等位基因缺失。结果表明,DPC4/SMAD4基因的两个等位基因失活发生在相当大比例的晚期结直肠癌中,DPC4/SMAD4基因可能在结直肠癌发生中发挥肿瘤抑制作用,符合Knudson [A.G.]提出的双击概念的标准Knudson,遗传癌症,癌基因和抗癌基因,癌症杂志,45(1985):1437-1443。
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