流式细胞术分析胃癌DNA定位。

Cytometry Pub Date : 2000-10-15
T Sugai, N Uesugi, W Habano, S Nakamura, T Suto, E Fujimaki, C Itoh
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摘要

尽管已有大量关于胃癌DNA倍性的研究报道,但尚未发现进展过程中非整倍性程度(DNA指数,DI)的差异。我们试图绘制进展过程中DIs的差异,以阐明非整倍体在胃癌中的作用。我们将检查的胃癌分为肠型(n = 88)和弥漫性(n = 48),然后分析136例胃癌(粘膜内癌42例;粘膜下癌,39岁;晚期癌症,55例)。此外,我们使用相同的粘膜下癌检查了粘膜和粘膜下病变的DNA倍体模式,以研究个体癌症的肿瘤进展。在两种类型的胃癌中观察到肿瘤内DNA倍体的差异。在肠型癌症中,由不同DI指示的多个亚克隆出现在胃癌的早期,而在弥漫性癌症中,多个亚克隆主要出现在晚期癌症中。尽管早期肠型癌症的DI在1.0和2.0之间变化很大,但在早期弥漫性癌症中,DI往往小于1.2。然而,在晚期胃癌中,两种组织学类型的DI分布相似。在肠型癌症中,高DI(>1.3)的非整倍体常见于粘膜病变。相比之下,只有低DI (
本文章由计算机程序翻译,如有差异,请以英文原文为准。
DNA mapping of gastric cancers using flow cytometric analysis.

Although numerous studies of gastric cancers on DNA ploidy have been reported, differences in the degree of aneuploidy (DNA index, DI) during progression have not been identified. We attempted to chart the differences in DIs during progression to clarify the role of aneuploidy in gastric cancers. We classified the gastric cancers examined into intestinal (n = 88) and diffuse (n = 48) types, and then analyzed 136 gastric cancers (intramucosal cancer, 42; submucosal cancer, 39; advanced cancer, 55) by flow cytometry using multiple sampling. In addition, we examined the DNA ploidy pattern of mucosal and submucosal lesions using the same submucosal cancers to study the tumor progression in individual cancers. Intratumoral DNA differences in DNA ploidy were observed in both types of gastric cancers. In intestinal-type cancers, multiple subclones indicated by a different DI occurred during the early stage of gastric cancers, whereas in diffuse-type cancers, multiple subclones were found primarily in advanced cancers. Although the DI varied widely in early intestinal-type cancers between 1.0 and 2.0, in early diffuse-type cancers, the DI tended to be less than 1.2. However, in advanced stage gastric cancers, the DI distribution was similar for both histological types. In intestinal-type cancers, high DI (>1.3) aneuploidy was frequently found in mucosal lesions. In contrast, only low DI (<1.2) aneuploid clones were observed in mucosal lesions of diffuse-type cancers. The present results suggest that high DI aneuploid tumor clones in intramucosal cancers acquire invasive ability when they progress to submucosal cancers, whereas DNA aneuploidy itself plays an important role in submucosal invasion of diffuse-type cancers.

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