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通过信使核糖核酸差异显示技术鉴定与K-1735小鼠黑色素瘤转移潜能相关的差异表达基因。

Identification of genes differentially expressed in association with metastatic potential of K-1735 murine melanoma by messenger RNA differential display.

作者信息

Hashimoto Y, Shindo-Okada N, Tani M, Takeuchi K, Toma H, Yokota J

机构信息

Biology Division, National Cancer Center Research Institute, Chuo-ku, Tokyo, Japan.

出版信息

Cancer Res. 1996 Nov 15;56(22):5266-71.

PMID:8912867
Abstract

To identify genes differentially expressed in association with the metastatic potential of K-1735 mouse melanoma cells, the mRNA differential display method was applied to compare mRNAs from high- and low-metastatic K-1735-derived cells. Three of the high- and three of the low-metastatic clones were used to reduce the false positives in the initial screening, and Southern blot screening against reverse transcription-PCR products was used to confirm that cDNA fragments detect differential expression between high- and low-metastatic cells. By using 256 different combinations of modified long arbitrary primers which provide broad screening of expressed genes, approximately 12,000 cDNA fragments were amplified from mRNA of each cell line. Among them, eight genes were identified as being expressed in either high- or low-metastatic cells using Northern blot analysis. Integrin alpha6 and two unknown genes were expressed in high-metastatic cells, whereas beta-tropomyosin, macrophage colony-stimulating factor, inhibin/activin betaB subunit, and two unknown genes were expressed in low-metastatic cells. These results indicate that the acquisition of metastatic potential in tumor cells was regulated by activation and/or inactivation of several specific genes, such as those for cell adhesion molecule, cytoskeletal protein, and growth factors.

摘要

为了鉴定与K - 1735小鼠黑色素瘤细胞转移潜能相关的差异表达基因,应用mRNA差异显示方法比较高转移和低转移的K - 1735衍生细胞的mRNA。使用三个高转移克隆和三个低转移克隆来减少初始筛选中的假阳性,并通过针对逆转录 - PCR产物的Southern印迹筛选来确认cDNA片段检测到高转移和低转移细胞之间的差异表达。通过使用256种不同组合的修饰长任意引物,这些引物可对表达基因进行广泛筛选,从每个细胞系的mRNA中扩增出约12,000个cDNA片段。其中,通过Northern印迹分析鉴定出八个基因在高转移或低转移细胞中表达。整合素α6和两个未知基因在高转移细胞中表达,而β - 原肌球蛋白、巨噬细胞集落刺激因子、抑制素/激活素βB亚基和两个未知基因在低转移细胞中表达。这些结果表明,肿瘤细胞转移潜能的获得受几种特定基因的激活和/或失活调节,如细胞粘附分子、细胞骨架蛋白和生长因子相关的基因。

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