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肝脏肿瘤启动剂结节藻毒素在原代培养大鼠肝细胞中对肿瘤坏死因子α基因和早期反应基因的表达。

Expression of the tumor necrosis factor alpha gene and early response genes by nodularin, a liver tumor promoter, in primary cultured rat hepatocytes.

作者信息

Sueoka E, Sueoka N, Okabe S, Kozu T, Komori A, Ohta T, Suganuma M, Kim S J, Lim I K, Fujiki H

机构信息

Saitama Cancer Center Research Institute, Japan.

出版信息

J Cancer Res Clin Oncol. 1997;123(8):413-9. doi: 10.1007/BF01372544.

Abstract

Nodularin is a new liver carcinogen possessing a potent tumor-promoting activity in rat liver, mediated through inhibition of protein phosphatases 1 and 2A, and a weak initiating activity. Since we previously reported evidence that nodularin up-regulated expression of the tumor necrosis factor alpha gene (TNF alpha) and early-response genes in rat liver after its i.p. administration, and since TNF alpha had tumor-promoting activity in vitro, it is possible that TNF alpha itself is involved in liver tumor promotion. We investigated whether hepatocytes themselves induce expression of the TNF alpha gene and early-response genes in primary cultured rat hepatocytes treated with nodularin. Like nodularin, microcystin-LR, which is another liver tumor promoter belonging to the okadaic acid class, strongly induced TNF alpha gene expression in rat hepatocytes, as well as TNF alpha release from those cells into the medium. On the other hand, 12-O-tetradecanoylphorbol-13-acetate, which has been reported to induce no tumor promotion in rat liver, induced no apparent expression of the TNF alpha gene in primary cultured rat hepatocytes. As for the expression of early-response genes, 1 microM nodularin or microcystin-LR induced expression of the c-jun, jun B, jun D, c-fos, fos B and fra-1 genes in the hepatocytes, and the expression of these genes was prolonged up to 24 h, suggesting mRNA stabilization induced by inhibition of protein phosphatases 1 and 2A. This paper presents new evidence that the TNF alpha gene and early-response genes were expressed in hepatocytes treated with a liver tumor promoter.

摘要

节球藻毒素是一种新型肝致癌物,在大鼠肝脏中具有强大的促肿瘤活性,其作用机制是抑制蛋白磷酸酶1和2A,且具有较弱的启动活性。由于我们之前报道过,腹腔注射节球藻毒素后,大鼠肝脏中肿瘤坏死因子α基因(TNFα)和早期反应基因的表达上调,并且由于TNFα在体外具有促肿瘤活性,因此TNFα本身可能参与了肝脏肿瘤的促进过程。我们研究了在经节球藻毒素处理的原代培养大鼠肝细胞中,肝细胞自身是否会诱导TNFα基因和早期反应基因的表达。与节球藻毒素一样,微囊藻毒素-LR(属于冈田酸类的另一种肝肿瘤促进剂)在大鼠肝细胞中强烈诱导TNFα基因表达,以及TNFα从这些细胞释放到培养基中。另一方面,据报道在大鼠肝脏中不具有促肿瘤作用的12-O-十四酰佛波醇-13-乙酸酯,在原代培养大鼠肝细胞中未诱导出明显的TNFα基因表达。至于早期反应基因的表达,1微摩尔节球藻毒素或微囊藻毒素-LR在肝细胞中诱导了c-jun、jun B、jun D、c-fos、fos B和fra-1基因的表达,并且这些基因的表达持续长达24小时,这表明蛋白磷酸酶1和2A的抑制诱导了mRNA的稳定。本文提供了新的证据,表明肝肿瘤促进剂处理的肝细胞中表达了TNFα基因和早期反应基因。

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