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与丁酸盐诱导人结肠癌细胞分化相关的pp60c-src和p56lck表达的改变。

Alterations in the expression of pp60c-src and p56lck associated with butyrate-induced differentiation of human colon carcinoma cells.

作者信息

Foss F M, Veillette A, Sartor O, Rosen N, Bolen J B

机构信息

Laboratory of Tumor Virus Biology, National Cancer Institute, Bethesda, Maryland 20892.

出版信息

Oncogene Res. 1989;5(1):13-23.

PMID:2476706
Abstract

The effects of butyrate-mediated differentiation of human colon carcinoma cells on the expression of src-related tyrosine protein kinases were analyzed. The results demonstrate that treatment of a variety of colon carcinoma cell lines with 2 mM sodium butyrate resulted in diminished population doubling rates, altered morphology, decreased anchorage-independent growth, and increased expression of colon epithelial differentiation marker enzymes such as alkaline phosphatase. In butyrate-treated cells, significantly diminished protein kinase activities and abundance of pp60c-src and p56lck were found to parallel the butyrate-induced phenotypic alterations. For the lck gene, the decreased levels in p56lck abundance were found to coincide with diminished levels of steady-state lck mRNAs. In contrast, treatments which arrested the growth of the colon carcinoma cells without inducing differentiation had no effect on the level of expression of these proteins. Furthermore, colon carcinoma cell lines which were found to be resistant to butyrate-induced differentiation showed no change in the kinase activity or abundance of either protein following butyrate treatment. These results indicate that the expression of several src-related kinases in human colon carcinoma can be influenced by the differentiation state of the cells.

摘要

分析了丁酸盐介导的人结肠癌细胞分化对src相关酪氨酸蛋白激酶表达的影响。结果表明,用2 mM丁酸钠处理多种结肠癌细胞系会导致群体倍增率降低、形态改变、非贴壁依赖性生长减少,以及结肠上皮分化标记酶如碱性磷酸酶的表达增加。在丁酸盐处理的细胞中,发现蛋白激酶活性显著降低,pp60c-src和p56lck的丰度与丁酸盐诱导的表型改变平行。对于lck基因,发现p56lck丰度的降低与稳态lck mRNA水平的降低相一致。相反,在不诱导分化的情况下阻止结肠癌细胞生长的处理对这些蛋白的表达水平没有影响。此外,发现对丁酸盐诱导的分化具有抗性的结肠癌细胞系在丁酸盐处理后,激酶活性或这两种蛋白的丰度均无变化。这些结果表明,人结肠癌中几种src相关激酶的表达可受细胞分化状态的影响。

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