[Effects of simvastatin on lipopolysaccharide induced α-subunit epithelial sodium channel mRNA in rat lung alveolar type II epithelial cells].

Pei-ying Liu, Dao-miao Xu
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Abstract

Objective: To study the impact of simvastatin on α-subunit epithelial sodium channel (α-ENaC) mRNA expression in primary culture alveolar typeII (ATII) epithelial cell of rats induced by lipopolysaccharide (LPS) in vitro.

Methods: ATII of primary generation were isolated from adult Sprague-Dawley (SD) rats. The cells were randomly divided into five groups: blank control group, LPS injured group (final concentration of LPS 1 mg/L), simvastatin low and high concentration groups (final concentration of simvastatin 20 μmol/L, 30 μmol/L, respectively), solution control group. Then, after being intervened for 1, 12 and 24 hours, the level of human tumor necrosis factor-α (TNF-α) and interleukin-1β (IL-1β) were monitored by enzyme-linked immunosorbent assay (ELISA), and α-ENaC mRNA expression was tested by reverse transcription-polymerase chain reaction (RT-PCR).

Results: After being intervened for 1, 12 and 24 hours, expressions of TNF-α and IL-1β in LPS injured group were obviously higher than those in blank control group. Expressions of TNF-α and IL-1β at 1, 12 and 24 hours in simvastatin low concentration group were significantly decreased compared with those in LPS injured group (TNF-α 1 hour: 1178.80±127.43 ng/L vs. 2336.00±170.04 ng/L, 12 hours: 1003.60±59.61 ng/L vs. 2479.80±210.41 ng/L, 24 hours: 695.80±25.24 ng/L vs. 1167.60±132.72 ng/L; IL-β 1 hour: 285.00±42.60 ng/L vs. 429.60±27.39 ng/L, 12 hours: 238.60±24.12 ng/L vs. 822.20±12.74 ng/L, 24 hours: 213.40±17.87 ng/L vs. 637.60±22.96 ng/L, all P<0.05). Expressions of TNF-α and IL-1β in high concentration group were decreased more obviously than those in low concentration group (TNF-α 1 hour: 965.60±24.45 ng/L vs. 1178.80±127.43 ng/L, 12 hours: 522.80±16.89 ng/L vs. 1003.60±59.61 ng/L, 24 hours: 252.40±17.64 ng/L vs. 695.80±25.24 ng/L; IL-1β 1 hour: 225.60±34.44 ng/L vs. 285.00±42.60 ng/L, 12 hours: 190.60±17.64 ng/L vs. 238.60±24.12 ng/L, 24 hours: 152.80±14.70 ng/L vs. 213.40±17.87 ng/L, all P<0.05), but increased compared with those in blank control group. After being intervened for 1 hour, no evident changes were observed in expression of α-ENaC mRNA in all groups. After being intervened for 12 hours and 24 hours, evident decrease in expression of α-ENaC mRNA (A value) was observed in LPS injured group compared with blank control group (12 hours: 0.211±0.021 vs. 0.496±0.027, 24 hours: 0.253±0.030 vs. 0.482±0.030, both P<0.05). Expressions of α-ENaC mRNA in simvastatin low concentration group evidently increased compared with those in LPS injured group (12 hours: 0.363±0.030 vs. 0.211±0.021, 24 hours: 0.309±0.024 vs. 0.253±0.030, both P<0.05). Expressions of α-ENaC mRNA in simvastatin high concentration group increased more obviously compared with those in low concentration group (12 hours: 0.413±0.034 vs. 0.363±0.030, 24 hours: 0.346±0.024 vs. 0.309±0.024, both P<0.05), but decreased compared with blank control group. No evident difference in expressions of all indexes in solution control group was observed compared with those in blank control group.

Conclusions: High dose simvastatin could improve α-ENaC mRNA expression in primary culture ATII epithelial cells of rats. This may act by modulation the level of TNF-α and IL-1β.

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辛伐他汀对脂多糖诱导的大鼠肺泡II型上皮细胞α-亚基上皮钠通道mRNA的影响。
目的:研究辛伐他汀对脂多糖(LPS)诱导大鼠肺泡ii型(ATII)上皮原代培养细胞α-亚单位上皮钠通道(α-ENaC) mRNA表达的影响。方法:从成年SD大鼠中分离第一代ATII。将细胞随机分为5组:空白对照组、LPS损伤组(LPS终浓度为1 mg/L)、辛伐他汀低、高浓度组(辛伐他汀终浓度分别为20、30 μmol/L)、溶液对照组。干预1、12、24 h后,采用酶联免疫吸附法(ELISA)检测人肿瘤坏死因子-α (TNF-α)、白细胞介素-1β (IL-1β)水平,采用逆转录聚合酶链反应(RT-PCR)检测α-ENaC mRNA表达。结果:干预1、12、24小时后,LPS损伤组TNF-α、IL-1β表达明显高于空白对照组。辛伐他汀低浓度组1、12、24小时TNF-α、IL-1β的表达均较LPS损伤组显著降低(TNF-α 1小时:1178.80±127.43 ng/L比2336.00±170.04 ng/L, 12小时:1003.60±59.61 ng/L比2479.80±210.41 ng/L, 24小时:695.80±25.24 ng/L比1167.60±132.72 ng/L;IL-β 1小时:285.00±42.60 ng/L vs. 429.60±27.39 ng/L, 12小时:238.60±24.12 ng/L vs. 822.20±12.74 ng/L, 24小时:213.40±17.87 ng/L vs. 637.60±22.96 ng/L。结论:大剂量辛伐他汀可提高原代培养大鼠ATII上皮细胞α-ENaC mRNA的表达。这可能通过调节TNF-α和IL-1β的水平起作用。
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