Allelic imbalance on the long arm of chromosome 21 in human oral squamous cell carcinoma: relationship between allelic imbalances (LOH and MSI) and clinicopathologic features.

IF 0.5 Q4 DENTISTRY, ORAL SURGERY & MEDICINE

Bulletin of Tokyo Dental College Pub Date : 2001-11-01 DOI:10.2209/TDCPUBLICATION.42.211

N. Yamamoto, H. Noma, T. Shibahara

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引用次数: 17

Abstract

Frequent allelic imbalances, including loss of heterozygosity (LOH) and microsatellite instability (MSI), have been found on the long arm of chromosome 21 (21q) in several types of human cancer. This study was designed to identify the tumor suppressor locus (or loci) associated with oral squamous cell carcinoma (SCC) on 21q. In order to understand the details of genetic alterations on chromosome 21, we performed polymerase chain reaction analysis of microsatellite polymorphisms corresponding to ten loci on this chromosome. We examined forty primary tumor tissues, forty corresponding normal tissues, and seven lymph node metastatic tissues. We identified novel tumor suppressor loci in this region in primary oral SCCs. To further determine the role of 21q deletions in oral cavity carcinogenesis, forty oral SCCs were examined for allelic imbalances (LOH or MSI) at 21q using ten microsatellite markers. Among these forty patients, twenty-six (65%) showed LOH at one or more loci. Deletion mapping of these tumors revealed four discrete, commonly deleted regions on the chromosome arm. Furthermore, we detected MSI in seventeen of those tested cases (42.5%). We compared our results with the clinicopathologic features. A number of sites displaying LOH at 21q could be detected in early stage lesions, and the frequencies of LOH tended to be higher in later clinical stages, but no statistical correlation was observed. Our results strongly suggest that allelic imbalances on 21q are involved in the development of oral SCC and that at least four different putative tumor suppressor genes contributing to the pathogenesis of this disease are present on 21q. Furthermore, allelic loss on 21q appears to be a useful indicator for evaluating the malignancy and prognosis of oral SCC, because the LOH of recurrent cases was more frequent than that of non-recurrent ones.

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人口腔鳞状细胞癌21号染色体长臂上的等位基因失衡:等位基因失衡(LOH和MSI)与临床病理特征的关系

在几种类型的人类癌症中，在21号染色体长臂(21q)上发现了常见的等位基因失衡，包括杂合性缺失(LOH)和微卫星不稳定性(MSI)。本研究旨在确定21q上与口腔鳞状细胞癌(SCC)相关的肿瘤抑制位点(或多个位点)。为了了解21号染色体遗传改变的细节，我们对该染色体上10个位点对应的微卫星多态性进行了聚合酶链反应分析。我们检查了40个原发肿瘤组织，40个相应的正常组织和7个淋巴结转移组织。我们在原发口腔SCCs的这一区域发现了新的肿瘤抑制位点。为了进一步确定21q缺失在口腔癌变中的作用，我们使用10个微卫星标记检测了40例口腔SCCs在21q处的等位基因失衡(LOH或MSI)。在这40例患者中，26例(65%)在一个或多个位点出现LOH。这些肿瘤的缺失图谱显示了染色体臂上四个离散的、通常缺失的区域。此外，我们在17例检测病例(42.5%)中检测到MSI。我们将结果与临床病理特征进行比较。在早期病变中可以检测到21q出现LOH的多个部位，在后期临床阶段LOH的频率趋于较高，但无统计学相关性。我们的研究结果强烈表明，21q上的等位基因失衡参与了口腔SCC的发展，并且至少有四种不同的推定肿瘤抑制基因存在于21q上，这些基因参与了这种疾病的发病机制。此外，21q上的等位基因缺失似乎是评估口腔SCC恶性程度和预后的有用指标，因为复发病例的LOH比非复发病例更频繁。

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来源期刊

Bulletin of Tokyo Dental College DENTISTRY, ORAL SURGERY & MEDICINE-

CiteScore

0.90

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0.00%

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期刊介绍： The bulletin of Tokyo Dental collegue is principally for the publication of original contributions to multidisciplinary research in dentistry.