Objective This study aimed to clarify the intervention effect of salidroside(SAL)on lung injury caused by PM_(2.5) in mice and illuminate the function of SIRT1-PGC-1ɑaxis.Methods Specific pathogen-free(SPF)grade male...Objective This study aimed to clarify the intervention effect of salidroside(SAL)on lung injury caused by PM_(2.5) in mice and illuminate the function of SIRT1-PGC-1ɑaxis.Methods Specific pathogen-free(SPF)grade male C57BL/6 mice were randomly assigned to the following groups:control group,SAL group,PM_(2.5) group,SAL+PM_(2.5) group.On the first day,SAL was given by gavage,and on the second day,PM_(2.5) suspension was given by intratracheal instillation.The whole experiment consist of a total of 10 cycles,lasting 20 days.At the end of treatment,blood samples and lung tissues were collected and analyzed.Observation of pathological changes in lung tissue using inverted microscopy and transmission electron microscopy.The expression of inflammatory,antioxidants,apoptosis,and SIRT1-PGC-1ɑproteins were detected by Western blotting.Results Exposure to PM_(2.5) leads to obvious morphological and pathologica changes in the lung of mice.PM_(2.5) caused a decline in levels of antioxidant-related enzymes and protein expressions of HO-1,Nrf2,SOD2,SIRT1 and PGC-1ɑ,and an increase in the protein expressions of IL-6,IL-1β,Bax,caspase-9 and cleaved caspase-3.However,SAL reversed the aforementioned changes caused by PM_(2.5) by activating the SIRT1-PGC-1α pathway.Conclusion SAL can activate SIRT1-PGC-1ɑ to ameliorate PM2.5-induced lung injury.展开更多
目的探讨沉默信息调节因子2相关酶1(silent mating type information regulation 2 homolog-1,SIRT1)抑制剂EX-527与激动剂SRT1720对老化内皮细胞成血管能力的影响。方法采用体外培养大鼠原代主动脉内皮细胞衰老技术,通过培养细胞的自...目的探讨沉默信息调节因子2相关酶1(silent mating type information regulation 2 homolog-1,SIRT1)抑制剂EX-527与激动剂SRT1720对老化内皮细胞成血管能力的影响。方法采用体外培养大鼠原代主动脉内皮细胞衰老技术,通过培养细胞的自然倍增建立大鼠主动脉内皮细胞(rat aorta endothelial cell,RAEC)衰老的细胞模型。内皮细胞的衰老用SA-β-Gal染色进行鉴定。衰老细胞模型建立后,对衰老的RAEC分别给予SIRT1抑制剂EX527和SIRT1激动剂SRT1720干预。运用Ki-67免疫荧光染色检测内皮细胞增殖,采用基质胶内皮管形成实验检测内皮细胞内皮管形成,应用蛋白印迹技术检测内皮细胞eNOS表达。结果SIRT1激动剂抑制老化RAEC增殖能力、内皮管形成能力和eNOS表达的降低,而SIRT1抑制剂使老化RAEC的增殖能力、内皮管形成能力和eNOS表达降低。结论SIRT1促进RAEC的增殖和内皮管形成,并增强RAEC中eNOS的表达;SIRT1改善衰老内皮细胞受损的成血管能力可能与其抑制衰老RAEC eNOS表达的下调有关。展开更多
基金supported by Shandong Provincial Natural Science Foundation,China(No.ZR2020MH336)Weifang Science and Technology Development Plan Project(NO.2022GX015,NO.2022GX010).
文摘Objective This study aimed to clarify the intervention effect of salidroside(SAL)on lung injury caused by PM_(2.5) in mice and illuminate the function of SIRT1-PGC-1ɑaxis.Methods Specific pathogen-free(SPF)grade male C57BL/6 mice were randomly assigned to the following groups:control group,SAL group,PM_(2.5) group,SAL+PM_(2.5) group.On the first day,SAL was given by gavage,and on the second day,PM_(2.5) suspension was given by intratracheal instillation.The whole experiment consist of a total of 10 cycles,lasting 20 days.At the end of treatment,blood samples and lung tissues were collected and analyzed.Observation of pathological changes in lung tissue using inverted microscopy and transmission electron microscopy.The expression of inflammatory,antioxidants,apoptosis,and SIRT1-PGC-1ɑproteins were detected by Western blotting.Results Exposure to PM_(2.5) leads to obvious morphological and pathologica changes in the lung of mice.PM_(2.5) caused a decline in levels of antioxidant-related enzymes and protein expressions of HO-1,Nrf2,SOD2,SIRT1 and PGC-1ɑ,and an increase in the protein expressions of IL-6,IL-1β,Bax,caspase-9 and cleaved caspase-3.However,SAL reversed the aforementioned changes caused by PM_(2.5) by activating the SIRT1-PGC-1α pathway.Conclusion SAL can activate SIRT1-PGC-1ɑ to ameliorate PM2.5-induced lung injury.
