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Microsatellite Instability in Gastric Intestinal Metaplasia in Patients with and without Gastric Cancer

机译:有和没有胃癌的患者肠胃上皮化生中的微卫星不稳定性

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摘要

The role and significance of microsatellite instability (MSI) in gastric carcinogenesis remain unknown. This study determined the chronology of MSI in gastric carcinogenesis by examining intestinal metaplasia (IM) from patients with and without gastric cancer. DNA was obtained from gastric specimens of 75 patients with gastric IM (30 cancer, 26 peptic ulcer, and 19 chronic gastritis patients) and was amplified with a set of eight microsatellite markers. Eight (26.7%) tumors and seven (9.3%) IM samples (three from cancer-free patients) displayed high-level MSI (three or more loci altered). Low-level MSI (one or two loci altered) was detected in 50% of the tumors, in 40% of IM samples coexisting with cancer, and in 38% of IM tissues of cancer-free individuals. Among the 30 cancer patients, microsatellites were more frequently altered in IM coexisting with tumors that showed MSI (P = 0.003). In addition, patients with low-level MSI in the tumor tissues were more likely to have active Helicobacter pylori infection than those with stable tumors (P = 0.02). In conclusion, this study indicates that MSI occurs not only in gastric IM of patients with gastric carcinoma, but also in IM of cancer-free individuals. These data suggest that the progressive accumulation of MSI in areas of IM may contribute to gastric cancer development, representing an important molecular event in the multistep gastric carcinogenesis cascade.
机译:微卫星不稳定性(MSI)在胃癌发生中的作用和意义仍然未知。这项研究通过检查有无胃癌患者的肠上皮化生(IM)来确定MSI在胃癌发生中的时间顺序。从75例患有胃IM的患者(30例癌症,26例消化性溃疡和19例慢性胃炎患者)的胃标本中获得DNA,并用一组8个微卫星标记进行扩增。八个(26.7%)肿瘤和七个(9.3%)IM样本(三个来自无癌患者)显示出高水平的MSI(三个或三个以上基因座已改变)。在50%的肿瘤,40%的与癌症共存的IM样本和38%的无癌个体的IM组织中检测到低水平的MSI(改变了一个或两个基因座)。在30例癌症患者中,微卫星在IM中与MSI并存的肿瘤中更频繁地发生改变(P = 0.003)。此外,肿瘤组织中MSI水平低的患者比稳定肿瘤的患者更有可能发生主动幽门螺杆菌感染(P = 0.02)。总之,这项研究表明,MSI不仅发生在胃癌患者的胃部IM中,而且还发生在无癌个体的IM中。这些数据表明MSI在IM区域的逐渐积累可能有助于胃癌的发展,这代表了多步胃癌发生级联反应中的重要分子事件。

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