他汀类药物调控 p38 丝裂原活化激酶介导的胎儿膜衰老。
Regulation of p38 mitogen-activated kinase-mediated fetal membrane senescence by statins.
机构信息
Department of Obstetrics & Gynecology, Division of Maternal-Fetal Medicine & Perinatal Research, The University of Texas Medical Branch at Galveston, Galveston, TX, USA.
Department of Epidemiology and Biostatistics, Texas A&M University Health Science Center, College Station, TX, USA.
出版信息
Am J Reprod Immunol. 2018 Oct;80(4):e12999. doi: 10.1111/aji.12999. Epub 2018 Jun 17.
PROBLEM
Oxidative stress (OS)-induced, p38 mitogen-activated protein kinase (p38MAPK)-mediated chorioamniotic senescence and inflammation (senescence-associated secretory phenotype [SASP]) are associated with parturition. In response to OS-inducing risk factors, premature senescence contributes to preterm premature rupture of the membranes (pPROM) and spontaneous preterm birth (PTB). We determined the effect of simvastatin, rosuvastatin, and progesterone in downregulating p38MAPK-mediated senescence and SASP.
METHOD OF STUDY
Normal term, not-in-labor fetal membranes (n = 8) were exposed to cigarette smoke extract (CSE: OS inducer) alone or combined with simvastatin (100 and 200 ng/mL), rosuvastatin (100 and 200 ng/mL), and progesterone (10 mol/L). p38MAPK expression changes were studied by Western blot, senescence was determined by senescence-associated β-Galactosidase (SA-β-Gal) staining, and multiplex analysis determined changes associated with 4 SASP markers (IL-8, IL-10, TNF-α, and GM-CSF). A pairwise comparison between groups was conducted by ANOVA.
RESULTS
Compared to untreated controls, CSE induced p38MAPK-mediated senescence and SASP. CSE cotreatment with simvastatin and rosuvastatin significantly reduced p38MAPK activation, senescence (decrease in SA-β-Gal) and SASP markers, GM-CSF, and TNF, but not IL-8, while increasing anti-inflammatory IL-10 in a dose-dependent manner. Cotreatment of CSE and progesterone had no effect on reducing p38MAPK activation, senescence, or SASP.
CONCLUSION
Both simvastatin and rosuvastatin downregulated OS-induced p38MAPK activation, senescence, and SASP, while rosuvastatin showed a pronounced effect. Progesterone did not reduce OS-induced fetal membrane senescence and SASP. Simvastatin or rosuvastatin may reduce the incidences of OS-associated PTB and pPROM by preventing premature senescence and SASP.
问题
氧化应激(OS)诱导的 p38 丝裂原活化蛋白激酶(p38MAPK)介导的绒毛膜羊膜炎衰老和炎症(衰老相关分泌表型[SASP])与分娩有关。在应对诱导 OS 的危险因素时,过早衰老会导致早产胎膜早破(pPROM)和自发性早产(PTB)。我们确定了辛伐他汀、罗苏伐他汀和孕酮下调 p38MAPK 介导的衰老和 SASP 的作用。
研究方法
正常足月、未分娩的胎儿胎膜(n=8)单独或联合暴露于香烟烟雾提取物(CSE:OS 诱导剂),或联合辛伐他汀(100 和 200ng/ml)、罗苏伐他汀(100 和 200ng/ml)和孕酮(10 摩尔/L)。通过 Western blot 研究 p38MAPK 表达变化,通过衰老相关 β-半乳糖苷酶(SA-β-Gal)染色测定衰老,通过多重分析测定与 4 个 SASP 标志物(IL-8、IL-10、TNF-α和 GM-CSF)相关的变化。通过方差分析进行组间两两比较。
结果
与未处理的对照组相比,CSE 诱导了 p38MAPK 介导的衰老和 SASP。CSE 与辛伐他汀和罗苏伐他汀联合治疗显著降低了 p38MAPK 激活、衰老(SA-β-Gal 减少)和 SASP 标志物 GM-CSF 和 TNF,但不包括 IL-8,同时呈剂量依赖性增加抗炎性 IL-10。CSE 和孕酮联合治疗对降低 p38MAPK 激活、衰老或 SASP 没有影响。
结论
辛伐他汀和罗苏伐他汀均可下调 OS 诱导的 p38MAPK 激活、衰老和 SASP,而罗苏伐他汀的作用更为显著。孕酮不能减少 OS 诱导的胎儿膜衰老和 SASP。辛伐他汀或罗苏伐他汀可能通过预防过早衰老和 SASP 来降低与 OS 相关的 PTB 和 pPROM 的发生率。
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