砷及其代谢物对BEAS-2B细胞p53基因表达影响
Effects of arsenic and its metabolites on p53 gene expression in BEAS-2B cells
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摘要:
背景 砷是人类致癌物。砷及其代谢物会影响
p53 表达,但砷及其代谢物处理人正常肺上皮细胞系(BEAS-2B)后,p53磷酸化及泛素化水平的变化尚不清楚。目的 探讨砷及其代谢物一甲基胂酸(MMA)和二甲基胂酸(DMA)对BEAS-2B细胞中抑癌基因
p53 表达的影响。方法 用不同浓度亚砷酸钠(NaAsO2)染毒细胞,利用CCK-8试剂检测细胞活力,确定NaAsO2染毒BEAS-2B细胞的剂量和时间。基于细胞活力结果,将细胞分为两组,即不同浓度亚砷酸钠组和砷甲基化代谢产物组,不同浓度亚砷酸钠组染毒剂量分别为0、2、4、6 μmol·L−1 NaAsO2;砷甲基化代谢产物组包括0 μmol·L−1 NaAsO2(对照组)、6 μmol·L−1 MMA组、6 μmol·L−1 DMA组和6 μmol·L−1 NaAsO2组。48 h收集细胞,提取总蛋白和总RNA,采用实时荧光定量聚合酶链式反应(qRT-PCR)检测
p53 mRNA相对表达水平,采用免疫共沉淀和蛋白质免疫印迹法检测p53泛素化水平,通过蛋白免疫印迹法检测p53蛋白、p53 Ser9和Ser15位点磷酸化蛋白的相对表达水平。结果 在BEAS-2B细胞中,与对照组相比,不同浓度NaAsO2染毒后,细胞存活率均降低(
P <0.05),并且NaAsO2浓度在6 μmol·L−1时细胞存活率约为50%。与对照组相比,不同浓度的NaAsO2(2、4、6 μmol·L−1)处理后p53 mRNA相对表达水平呈逐渐降低趋势,差异具有统计学意义(P <0.05);不同浓度的NaAsO2诱导p53蛋白、Ser9位点磷酸化蛋白相对表达水平均逐渐降低(P <0.05);不同浓度的NaAsO2诱导p53 Ser15位点磷酸化蛋白相对表达水平均呈逐渐降低趋势,但仅6 μmol·L−1NaAsO2组低于对照组且差异具有统计学意义(P <0.05)。与对照组相比,MMA组和DMA组p53 mRNA、p53蛋白、Ser9和Ser15位点磷酸化蛋白相对表达水平无明显影响。与对照组相比,NaAsO₂染毒后,p53泛素化表达水平明显下降,K48位点泛素化表达水平下降。结论 砷引起BEAS-2B细胞p53蛋白表达降低主要由于其磷酸化途径被抑制和mRNA表达降低,p53泛素化水平减少所致的蛋白变化未占主导作用。MMA和DMA对
p53 基因表达无影响。Abstract:Background Arsenic is a human carcinogen. Arsenic and its metabolites affect the expression of
p53 , but whether there are any changes of p53 phosphorylation and ubiquitination levels in human bronchial epithelium cells (BEAS-2B) are not clear after exposure to arsenic and its metabolites.Objective To study the effects of arsenic and its metabolites monomethylarsic acid (MMA) and dimethylarsinic acid (DMA) on the expression of tumor suppressor gene
p53 in BEAS-2B cells.Methods Different concentrations of sodium arsenite (NaAsO2) were used to infect BEAS-2B cells, and the cell viability was detected with CCK-8 reagent to determine the dose and time of NaAsO2 used for the following study. Based on the results of cell viability, the cells were divided into two panels: a sodium arsenide panel and an arsenic methylation metabolite penal. The doses of sodium arsenite were 0, 2, 4, and 6 μmol·L−1 NaAsO2; the arsenic methylation metabolite panel consisted of 0 μmol·L−1 NaAsO2 group (control), 6 μmol· L−1 MMA group, 6 μmol· L−1 DMA group, and 6 μmol· L−1 NaAsO2 group. The cells were collected after 48 h treatment, and the total protein and total RNA were extracted. The relative levels of
p53 mRNA expression were determined by quantitative real-time polymerase chain reaction (qRT-PCR), the relative expression levels of p53 protein, p53 Ser9 and Ser15 phosphorylated proteins were determined by Western blot, and the level of p53 ubiquitination was detected by co-immunoprecipitation (CO-IP).Results Compared with the control group, the cell viability rates in all BEAS-2B cells treated by NaAsO2 were significantly reduced (
P <0.05), and the 50% cell viability was observed at 6 μmol·L−1. Compared with the control group, the relative expression level ofp53 mRNA gradually decreased after NaAsO2 (2, 4, 6 μmol·L−1) treatment (P <0.05), the relative expression levels of p53 protein and Ser9 phosphorylated protein induced by NaAsO2 also decreased gradually (P <0.05), and the relative expression level of p53 Ser15 phosphorylated protein induced by NaAsO2 followed the same pattern, but it was only lower than that of the control group in the 6 μmol·L−1 NaAsO2 group (P <0.05). Compared with the control group, there were no significant effects on the relative expression levels ofp53 mRNA, p53 protein, Ser9 and Ser15 phosphorylated proteins in the MMA group and the DMA group. Compared with the control group, the expression level of p53 ubiquitination was significantly decreased and the expression of K48 ubiquitination decreased significantly after NaAsO2 infection.Conclusion Arsenic causes a decrease in the expression of the p53 protein in BEAS-2B cells, largely due to inhibition of the phosphorylated pathway and a decrease in mRNA expression, and protein changes caused by a decrease in p53 ubiquitination do not play a dominant role. MMA and DMA do not affect
p53 gene expression.
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