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通过cDNA宏阵列检测人结直肠癌组织中血管生成基因表达上调及细胞周期基因表达下调。

Upregulated expression of angiogenesis genes and down regulation of cell cycle genes in human colorectal cancer tissue determined by cDNA macroarray.

作者信息

Tsunoda T, Nakamura T, Ishimoto K, Yamaue H, Tanimura H, Saijo N, Nishio K

机构信息

Second Department of Surgery, Wakayama Medical School, 811-1 Kimiidera, Wakayama, 641-0012, Japan.

出版信息

Anticancer Res. 2001 Jan-Feb;21(1A):137-43.

Abstract

The differential expression of hundreds of tightly, transcriptionally controlled genes in isolated human colorectal cancer and respective normal mucosa from two patients was analyzed by the cDNA macroarray technique. mRNA prepared from the colorectal cancer tumors was compared with 588 genes spotted onto the filter. Case A showed down-regulation of the expression of cell-cycle-related genes including cyclins, cyclin-dependent kinase (CDK) 2, and CDK-activating kinase, as compared with normal mucosa from the same patient. The tumors showed up-regulation of expression of angiogenesis-related genes such as type II cytoskeletal 8 keratin, metalloproteinase subtypes, VEGF, and bFGF, to over 5-fold the levels in normal mucosa. Thus, colorectal carcinoma tissues are characterized by the upregulation of molecules related with angiogenesis. These results suggest that angiogenesis-related molecules are suitable candidates for target-based therapies for colorectal cancer patients. In case B, the largest difference in expression between the tumor and mucosal tissues was observed in the MMP-1 gene. In contrast to the first case, there was no increase in expression of angiogenesis-related molecules or decrease in expression of cell-cycle-regulatory molecules. The expression profile was quite different between these two patients. This approach may eventually provide a mean of selecting target-based drugs in individual colon cancer patients.

摘要

采用cDNA宏阵列技术分析了两名患者分离出的人结肠直肠癌及相应正常黏膜中数百个受到严格转录调控的基因的差异表达。将从结肠直肠癌肿瘤中制备的mRNA与点样于滤膜上的588个基因进行比较。病例A显示,与同一患者的正常黏膜相比,细胞周期相关基因(包括细胞周期蛋白、细胞周期蛋白依赖性激酶(CDK)2和CDK激活激酶)的表达下调。肿瘤中血管生成相关基因(如II型细胞骨架8角蛋白、金属蛋白酶亚型、血管内皮生长因子(VEGF)和碱性成纤维细胞生长因子(bFGF))的表达上调,达到正常黏膜水平的5倍以上。因此,结肠直肠癌组织的特征是与血管生成相关的分子上调。这些结果表明,血管生成相关分子是结肠癌患者基于靶点治疗的合适候选分子。在病例B中,肿瘤组织与黏膜组织之间表达差异最大的是基质金属蛋白酶-1(MMP-1)基因。与第一个病例不同,血管生成相关分子的表达没有增加,细胞周期调节分子的表达也没有减少。这两名患者的表达谱差异很大。这种方法最终可能为个体结肠癌患者选择基于靶点的药物提供一种手段。

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