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作 者:李梅华[1] 钟小宁[1] 柳广南[1] 何志义[1] 朱敏[2] 周刚[2]
机构地区:[1]广西医科大学第一附属医院呼吸内科,南宁530021 [2]中南大学湘雅医学院分子生物学研究中心
出 处:《广西医科大学学报》2010年第3期348-350,共3页Journal of Guangxi Medical University
基 金:广西自然科学基金资助项目(No.桂科自0229024)
摘 要:目的:从分子水平上探讨红霉素(EM)的抗炎作用机制,为临床防治慢性阻塞性肺疾病提供新的思路。方法:体外培养人支气管上皮细胞(16HBE),将细胞随机分为8组,先加入EM干预,后加入肿瘤坏死因子(TNF-α)刺激。分组:①空白对照组;②TNF-α(20μg/L,16h);③EM(0.3mg/L,24h)+TNF-α(20μg/L,16h);④EM(3mg/L,24h)+TNF-α(20μg/L,16h);⑤EM(30mg/L,24h)+TNF-α(20μg/L,16h);⑥EM(0.3mg/L,48h)+TNF-α(20μg/L,16h)。然后收集各组细胞分别提取核蛋白,应用电泳迁移率改变分析法(EMSA)检测核因子-κB(NF-κB)的活性。结果:EMSA结果显示,TNF-α刺激人支气管上皮细胞(16HBE)后,细胞内NF-κB表达增高。先加入不同浓度及作用时间的EM,后加入前炎因子TNF-α刺激16HBE,EMSA结果显示各组细胞NF-κB表达均降低,且提示有随着EM浓度增加,作用时间延长,NF-κB表达受抑制愈明显的趋势,但随着EM浓度增加及作用时间延长到一定的范围,NF-κB表达受抑制差别不明显。结论:TNF-α能激活16HBENF-κB,促进炎症的发生发展,在炎症进程中发挥着重要作用。EM能抑制人16HBENF-κB的激活水平,这可能是EM的抗炎作用机制之一。Objective: To investigate the anti-inflammatory molecular mechanism of erythromycin (EM) in order to find a new way to prevent and treat chronic obstructive pulmonary disease. Methods: Human bronchial epithelial cell line 16HBE was cultured with 10% serum DMEM(high glucose). The cells were randomly divided into eight groups : (1)control group;(2)tumor necrosis factor (TNF-α)(20 μg/L, 16 h);(2)EM (0. 3 mg/L,24 h)+TNF-α(20 μg/L,16 h);(4)EM(3 mg/L,24 h)4-TNF-α(20 μg/L,16 h);(5)EM(30 mg/ L,24 h)+TNF-α(20 μg/L,16 h) ;(6)EM(0.3 Mg/L,48 h)+TNF-α(20 μg/L,16 h). The cells were incubated with various concentrations of EM for 24~48 hours before the stimulation by TNF-α. The cellular nuclear protein was isolated to detect the activity of nuclear factor-kappa B(NF-κB)by applying electrophoresis mobility shift assay (EMSA). Results: The activation of NF-κB in human bronchial epithelial cell line 16HBE induced by TNF-α was inhibited by the preincubation with erythromycin in dose-dependent and time-dependent fashion. Conclusion: Our results indicate that erythromycin can modify inflammation presumably by suppressing the activation of NF-κB in human bronchial epithelial cells.
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