Accumulating evidence suggests that oxidative stress and the Wnt/β-catenin pathway participate in stroke-induced disruption of the blood-brain barrier.However,the potential links between them following ischemic strok...Accumulating evidence suggests that oxidative stress and the Wnt/β-catenin pathway participate in stroke-induced disruption of the blood-brain barrier.However,the potential links between them following ischemic stroke remain largely unknown.The present study found that cerebral ischemia leads to oxidative stress and repression of the Wnt/β-catenin pathway.Meanwhile,Wnt/β-catenin pathway activation by the pharmacological inhibito r,TWS119,relieved oxidative stress,increased the levels of cytochrome P4501B1(CYP1B1)and tight junction-associated proteins(zonula occludens-1[ZO-1],occludin and claudin-5),as well as brain microvascular density in cerebral ischemia rats.Moreove r,rat brain microvascular endothelial cells that underwent oxygen glucose deprivation/reoxygenation displayed intense oxidative stress,suppression of the Wnt/β-catenin pathway,aggravated cell apoptosis,downregulated CYP1B1and tight junction protein levels,and inhibited cell prolife ration and migration.Overexpression ofβ-catenin or knockdown ofβ-catenin and CYP1B1 genes in rat brain mic rovascular endothelial cells at least partly ameliorated or exacerbated these effects,respectively.In addition,small interfering RNA-mediatedβ-catenin silencing decreased CYP1B1 expression,whereas CYP1B1 knoc kdown did not change the levels of glycogen synthase kinase 3β,Wnt-3a,andβ-catenin proteins in rat brain microvascular endothelial cells after oxygen glucose deprivatio n/reoxygenation.Thus,the data suggest that CYP1B1 can be regulated by Wnt/β-catenin signaling,and activation of the Wnt/β-catenin/CYP1B1 pathway contributes to alleviation of oxidative stress,increased tight junction levels,and protection of the blood-brain barrier against ischemia/hypoxia-induced injury.展开更多
目的了解中国人群原发性先天性青光眼患者CYP1B1基因突变及其分布情况。方法检索Pub Med、Web of Science、CNKI、万方等数据库,收集公开发表的有关中国人群原发性先天性青光眼患者CYP1B1基因突变筛查研究文献。采用系统评价的方法评价...目的了解中国人群原发性先天性青光眼患者CYP1B1基因突变及其分布情况。方法检索Pub Med、Web of Science、CNKI、万方等数据库,收集公开发表的有关中国人群原发性先天性青光眼患者CYP1B1基因突变筛查研究文献。采用系统评价的方法评价文献质量,提取相关数据,运用Freeman-Tukey双反正弦变换法对基因突变率进行合并计算,收集并获得我国原发性先天性青光眼患者的CYP1B1基因突变谱。结果共纳入9篇文献,包括434例原发性先天性青光眼患者,其中69例存在CYP1B1基因突变,合并突变率为15.2%(95%可信区间11.8%~19.0%)。共发现43种突变,基因突变谱分散,以7990C〉T(L385F)、8006G〉A(R390H)、4124C〉G(L107V)三种突变频率最高,比较发现L107V是中国原发性先天性青光眼人群CYP1B1基因特有的变异位点。结论中国原发性先天性青光眼患者的CYP1B1基因突变率较低,提示该人群中存在除CYP1B1基因以外的其他致病基因。收集获得的CYP1B1基因突变谱可为今后原发性先天性青光眼人群基因突变筛查提供参考。展开更多
基金supported by the National Natural Science Foundation of China,No.81771250(to XC)the Natural Science Foundation of Fujian Province,Nos.2020J011059(to XC),2020R1011004(to YW),2021J01374(to XZ)+1 种基金Medical Innovation Project of Fujian Province,No.2021 CXB002(to XC)Fujian Research and Training Grants for Young and Middle-aged Leaders in Healthcare(to XC)。
文摘Accumulating evidence suggests that oxidative stress and the Wnt/β-catenin pathway participate in stroke-induced disruption of the blood-brain barrier.However,the potential links between them following ischemic stroke remain largely unknown.The present study found that cerebral ischemia leads to oxidative stress and repression of the Wnt/β-catenin pathway.Meanwhile,Wnt/β-catenin pathway activation by the pharmacological inhibito r,TWS119,relieved oxidative stress,increased the levels of cytochrome P4501B1(CYP1B1)and tight junction-associated proteins(zonula occludens-1[ZO-1],occludin and claudin-5),as well as brain microvascular density in cerebral ischemia rats.Moreove r,rat brain microvascular endothelial cells that underwent oxygen glucose deprivation/reoxygenation displayed intense oxidative stress,suppression of the Wnt/β-catenin pathway,aggravated cell apoptosis,downregulated CYP1B1and tight junction protein levels,and inhibited cell prolife ration and migration.Overexpression ofβ-catenin or knockdown ofβ-catenin and CYP1B1 genes in rat brain mic rovascular endothelial cells at least partly ameliorated or exacerbated these effects,respectively.In addition,small interfering RNA-mediatedβ-catenin silencing decreased CYP1B1 expression,whereas CYP1B1 knoc kdown did not change the levels of glycogen synthase kinase 3β,Wnt-3a,andβ-catenin proteins in rat brain microvascular endothelial cells after oxygen glucose deprivatio n/reoxygenation.Thus,the data suggest that CYP1B1 can be regulated by Wnt/β-catenin signaling,and activation of the Wnt/β-catenin/CYP1B1 pathway contributes to alleviation of oxidative stress,increased tight junction levels,and protection of the blood-brain barrier against ischemia/hypoxia-induced injury.
文摘目的了解中国人群原发性先天性青光眼患者CYP1B1基因突变及其分布情况。方法检索Pub Med、Web of Science、CNKI、万方等数据库,收集公开发表的有关中国人群原发性先天性青光眼患者CYP1B1基因突变筛查研究文献。采用系统评价的方法评价文献质量,提取相关数据,运用Freeman-Tukey双反正弦变换法对基因突变率进行合并计算,收集并获得我国原发性先天性青光眼患者的CYP1B1基因突变谱。结果共纳入9篇文献,包括434例原发性先天性青光眼患者,其中69例存在CYP1B1基因突变,合并突变率为15.2%(95%可信区间11.8%~19.0%)。共发现43种突变,基因突变谱分散,以7990C〉T(L385F)、8006G〉A(R390H)、4124C〉G(L107V)三种突变频率最高,比较发现L107V是中国原发性先天性青光眼人群CYP1B1基因特有的变异位点。结论中国原发性先天性青光眼患者的CYP1B1基因突变率较低,提示该人群中存在除CYP1B1基因以外的其他致病基因。收集获得的CYP1B1基因突变谱可为今后原发性先天性青光眼人群基因突变筛查提供参考。