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丁酸钠诱导人结肠直肠癌中癌胚抗原基因的表达。

Induction of carcinoembryonic-antigen-gene expression in human colorectal carcinoma by sodium butyrate.

作者信息

Saini K, Steele G, Thomas P

机构信息

Department of Surgery, New England Deaconess Hospital, Harvard Medical School, Boston, MA 02115.

出版信息

Biochem J. 1990 Dec 1;272(2):541-4. doi: 10.1042/bj2720541.

Abstract

The effect of sodium butyrate on the expression of the carcinoembryonic-antigen (CEA) gene was studied in two poorly differentiated colorectal-carcinoma cell lines (Clone-A and MIP-101) and in one well-differentiated cell line (LS-174T); A.T.C.C. no. CCL 188). Northern-blot and dot-blot analyses indicated a steady increase in CEA mRNA from day 4 to a maximal level by day 14 after these cells were exposed to 2 mM-sodium butyrate. Studies using nuclear run-off assays followed by dot-blot hybridization to a partial CEA cDNA clone demonstrated that specific increases in gene transcription rates (3-fold in MIP-101, 4-fold in LS-174T and 6-fold in Clone-A) are not sufficient to account for the observed increases in CEA mRNA abundance. Further studies showed that CEA-specific transcripts have a half-life of about 60-80 min, and treatment with sodium butyrate increased the stability of CEA-specific transcripts to about 340 min in LS-174T cells and to about 500 min in Clone-A cells. We conclude that the induction of the CEA-gene expression by sodium butyrate in colorectal-cancer cells is mediated by both transcriptional and post-transcriptional mechanisms, with CEA mRNA stability as one of the major check-points.

摘要

在两种低分化结肠癌细胞系(克隆-A和MIP-101)以及一种高分化细胞系(LS-174T;美国典型培养物保藏中心编号CCL 188)中研究了丁酸钠对癌胚抗原(CEA)基因表达的影响。Northern印迹和斑点印迹分析表明,这些细胞暴露于2 mM丁酸钠后,CEA mRNA从第4天开始稳步增加,到第14天达到最高水平。使用核转录分析,随后与部分CEA cDNA克隆进行斑点印迹杂交的研究表明,基因转录率的特异性增加(MIP-101中为3倍,LS-174T中为4倍,克隆-A中为6倍)不足以解释观察到的CEA mRNA丰度的增加。进一步的研究表明,CEA特异性转录本的半衰期约为60-80分钟,丁酸钠处理使LS-174T细胞中CEA特异性转录本的稳定性增加到约340分钟,在克隆-A细胞中增加到约500分钟。我们得出结论,丁酸钠在结肠癌细胞中诱导CEA基因表达是由转录和转录后机制介导的,其中CEA mRNA稳定性是主要检查点之一。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/505c/1149736/553af9c42a24/biochemj00170-0256-a.jpg

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