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首页> 外文期刊>Journal of Pathology: Journal of the Pathological Society of Great Britain and Ireland >Microsatellite instability in intestinal- and diffuse-type gastric carcinoma.
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Microsatellite instability in intestinal- and diffuse-type gastric carcinoma.

机译:肠型和弥漫型胃癌中的微卫星不稳定性。

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摘要

To investigate the role of genetic instability in the development of intestinal- and diffuse-type gastric cancers, six microsatellite loci were analysed in 98 carcinomas of the two main histotypes, at both early and advanced stages of progression, and in five preneoplastic lesions. RER+ phenotype frequency proved to be significantly higher (P = 0.013) in intestinal (23 per cent) than in diffuse cancers (5 per cent) and slightly higher in advanced (19 per cent) than in early (12 per cent) tumours. When comparing early and advanced tumours of the same histotype, a similar frequency was found for diffuse tumours (4 per cent vs. 6 per cent), and an increase from 19 to 30 per cent for intestinal cancers. Instability at more than one locus was limited to intestinal tumours and replication errors were also detected in an intestinal dysplasia. On the whole, these data suggest that genetic instability has an important and early role in gastric carcinogenesis of the intestinal type and a less important role in gastric carcinogenesis of the diffuse type. Most tumours of this panel had previously been characterized for p53 gene mutations. p53 screening was extended to all samples, to investigate the possible association between gene mutations and microsatellite instability. Analysis showed a trend (P = 0.07, Fisher's exact test) towards a negative association between these two genetic lesions in tumours of the intestinal type.
机译:为了研究遗传不稳定性在肠型和弥漫型胃癌发展中的作用,分析了两种主要组织型的98种癌的六个微卫星基因座,包括进展的早期和晚期,以及五个癌变前病变。事实证明,肠道(23%)的RER +表型频率显着高于弥漫性癌症(5%),而晚期(19%)比早期(12%)更高。比较相同组织类型的早期和晚期肿瘤时,发现弥漫性肿瘤的发生率相似(4%比6%),肠道癌从19%增至30%。在一个以上位点的不稳定性仅限于肠肿瘤,并且在肠发育不良中也检测到复制错误。总体而言,这些数据表明,遗传不稳定性在肠型胃癌的发生中起着重要的早期作用,而在弥散型胃癌的发生中起着不重要的作用。该小组的大多数肿瘤先前已针对p53基因突变进行了表征。 p53筛选扩展到所有样品,以研究基因突变与微卫星不稳定性之间的可能联系。分析显示在肠道型肿瘤中这两个遗传损伤之间呈负相关的趋势(P = 0.07,Fisher精确检验)。

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