基于24Model-D-ISM的地铁站火灾疏散影响因素研究

为预防地铁站火灾事故,深入了解地铁站火灾人员疏散影响因素间的内在联系与层次结构,基于第6版“2-4”模型(24Model)分析63起地铁站火灾疏散事故,充分考虑各个因素之间的交互作用,提取19个影响地铁站人员疏散的关键因素,建立地铁站火灾人员疏散影响因素指标体系;采用算子客观赋权法(C-OWA)改进决策试验与评价实验法(DEMATEL),确定地铁站火灾人员疏散的重要影响因素;在此基础上,采用解释结构模型(ISM)分析各个因素间的层次结构及相互作用路径,构建地铁站火灾人员疏散影响因素的多级递阶结构模型。研究结果表明:疏散引导、恐慌从众行为、人员拥挤为地铁站火灾人员疏散的关键影响因素;地铁站火灾人员疏散受表层因素、中间层因素、深层因素共同作用的影响,其中,疏散教育与培训、设施维护与检查、疏散预案等因素是根源影响因素,重视根源影响因素的改善有利于从本质上预防和控制事故的发生。

Long non-coding RNA H19 regulates neurogenesis of induced neural stem cells in a mouse model of closed head injury

Stem cell-based therapies have been proposed as a potential treatment for neural regeneration following closed head injury.We previously reported that induced neural stem cells exert beneficial effects on neural regeneration via cell replacement.However,the neural regeneration efficiency of induced neural stem cells remains limited.In this study,we explored differentially expressed genes and long non-coding RNAs to clarify the mechanism underlying the neurogenesis of induced neural stem cells.We found that H19 was the most downregulated neurogenesis-associated lnc RNA in induced neural stem cells compared with induced pluripotent stem cells.Additionally,we demonstrated that H19 levels in induced neural stem cells were markedly lower than those in induced pluripotent stem cells and were substantially higher than those in induced neural stem cell-derived neurons.We predicted the target genes of H19 and discovered that H19 directly interacts with mi R-325-3p,which directly interacts with Ctbp2 in induced pluripotent stem cells and induced neural stem cells.Silencing H19 or Ctbp2 impaired induced neural stem cell proliferation,and mi R-325-3p suppression restored the effect of H19 inhibition but not the effect of Ctbp2 inhibition.Furthermore,H19 silencing substantially promoted the neural differentiation of induced neural stem cells and did not induce apoptosis of induced neural stem cells.Notably,silencing H19 in induced neural stem cell grafts markedly accelerated the neurological recovery of closed head injury mice.Our results reveal that H19 regulates the neurogenesis of induced neural stem cells.H19 inhibition may promote the neural differentiation of induced neural stem cells,which is closely associated with neurological recovery following closed head injury.

Single-neuron neurodegeneration as a degenerative model for Parkinson’s disease

The positive effect of levodopa in the treatment of Parkinson’s disease,although it is limited in time and has severe side effects,has encouraged the scientific community to look for new drugs that can stop the neurodegenerative process or even regenerate the neuromelanin-containing dopaminergic nigrostriatal neurons.Successful preclinical studies with coenzyme Q10,mitoquinone,isradipine,nilotinib,TCH346,neurturin,zonisamide,deferiprone,prasinezumab,and cinpanemab prompted clinical trials.However,these failed and after more than 50 years levodopa continues to be the key drug in the treatment of the disease,despite its severe side effects after 4–6 years of chronic treatment.The lack of translated successful results obtained in preclinical investigations based on the use of neurotoxins that do not exist in the human body as new drugs for Parkinson’s disease treatment is a big problem.In our opinion,the cause of these failures lies in the experimental animal models involving neurotoxins that do not exist in the human body,such as 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine and 6-hydroxydopamine,that induce a very fast,massive and expansive neurodegenerative process,which contrasts with the extremely slow one of neuromelanin-containing dopaminergic neurons.The exceedingly slow progress of the neurodegenerative process of the nigrostriatal neurons in idiopathic Parkinson’s patients is due to(i)a degenerative model in which the neurotoxic effect of an endogenous neurotoxin affects a single neuron,(ii)a neurotoxic event that is not expansive and(iii)the fact that the neurotoxin that triggers the neurodegenerative process is produced inside the neuromelanin-containing dopaminergic neurons.The endogenous neurotoxin that fits this degenerative model involving one single neuron at a time is aminochrome,since it(i)is generated within neuromelanin-containing dopaminergic neurons,(ii)does not cause an expansive neurotoxic effect and(iii)triggers all the mechanisms involved in the neurodegenerative process of the nigrostriatal neurons in idiopathic Parkinson’s disease.In conclusion,based on the hypothesis that the neurodegenerative process of idiopathic Parkinson’s disease corresponds to a single-neuron neurodegeneration model,we must search for molecules that increase the expression of the neuroprotective enzymes DT-diaphorase and glutathione transferase M2-2.It has been observed that the activation of the Kelch-like ECH-associated protein 1/nuclear factor(erythroid-derived 2)-like 2 pathway is associated with the transcriptional activation of the DT-diaphorase and glutathione transferase genes.

MiR-142-3p Regulates ILC1s by Targeting HMGB1 via the NF-κB Pathway in a Mouse Model of Early Pregnancy Loss

Objective Innate lymphoid cells(ILCs)are a class of newly discovered immunocytes.Group 1 ILCs(ILC1s)are identified in the decidua of humans and mice.High mobility group box 1(HMGB1)is predicted to be one of the target genes of miR-142-3p,which is closely related to pregnancy-related diseases.Furthermore,miR-142-3p and HMGB1 are involved in regulating the NF-κB signaling pathway.This study aimed to examine the regulatory effect of miR-142-3p on ILC1s and the underlying mechanism involving HMGB1 and the NF-κB signaling pathway.Methods Mouse models of normal pregnancy and abortion were constructed,and the alterations of ILC1s,miR-142-3p,ILC1 transcription factor(T-bet),and pro-inflammatory cytokines of ILC1s(TNF-α,IFN-γand IL-2)were detected in mice from different groups.The targeting regulation of HMGB1 by miR-142-3p in ILC1s,and the expression of HMGB1 in normal pregnant mice and abortive mice were investigated.In addition,the regulatory effects of miR-142-3p and HMGB1 on ILC1s were detected in vitro by CCK-8,Annexin-V/PI,ELISA,and RT-PCR,respectively.Furthermore,changes of the NF-κB signaling pathway in ILC1s were examined in the different groups.For the in vivo studies,miR-142-3p-Agomir was injected in the uterus of abortive mice to evaluate the abortion rate and alterations of ILC1s at the maternal-fetal interface,and further detect the expression of HMGB1,pro-inflammatory cytokines,and the NF-κB signaling pathway.Results The number of ILC1s was significantly increased,the level of HMGB1 was significantly upregulated,and that of miR-142-3p was considerably downregulated in the abortive mice as compared with the normal pregnant mice(all P<0.05).In addition,miR-142-3p was found to drastically inhibit the activation of the NF-κB signaling pathway(P<0.05).The number of ILC1s and the levels of pro-inflammatory cytokines were significantly downregulated and the activation of the NF-κB signaling pathway was inhibited in the miR-142-3p Agomir group(all P<0.05).Conclusion miR-142-3p can regulate ILC1s by targeting HMGB1 via the NF-κB signaling pathway,and attenuate the inflammation at the maternal-fetal interface in abortive mice.

Fuzzy-Model-Based Finite Frequency Fault Detection Filtering Design for Two-Dimensional Nonlinear Systems

This article studies the fault detection filtering design problem for Roesser type two-dimensional(2-D)nonlinear systems described by uncertain 2-D Takagi-Sugeno(T-S)fuzzy models.Firstly,fuzzy Lyapunov functions are constructed and the 2-D Fourier transform is exploited,based on which a finite frequency fault detection filtering design method is proposed such that a residual signal is generated with robustness to external disturbances and sensitivity to faults.It has been shown that the utilization of available frequency spectrum information of faults and disturbances makes the proposed filtering design method more general and less conservative compared with a conventional nonfrequency based filtering design approach.Then,with the proposed evaluation function and its threshold,a novel mixed finite frequency H_(∞)/H_(-)fault detection algorithm is developed,based on which the fault can be immediately detected once the evaluation function exceeds the threshold.Finally,it is verified with simulation studies that the proposed method is effective and less conservative than conventional non-frequency and/or common Lyapunov function based filtering design methods.

基于SPI-RRV指数中国气象干旱及其风险时空演变特征研究

为全面揭示变化环境下我国多维气象干旱特征,耦合气象干旱指数(SPI)和可靠性-回弹性-脆弱性(RRV)指数,提出了一种基于SPI-RRV指数的干旱风险评价方法,定量评价了中国气象干旱及其风险的时空演变特征。结果表明:SPI-RRV指数具有特征稳定和时空可比性强的特点,能够较为准确地评估气象干旱风险时空演变特征;南方平均干旱栅格比、干旱月占比和频次大于北方,湿润区和半湿润区干旱历时短、烈度大,半干旱区和干旱区干旱历时长、烈度相对较小;干旱高风险区转移具有显著年代际变化规律,空间上从西北向西南地区转移。

深部煤储层孔裂隙结构对煤层气赋存的影响-以鄂尔多斯盆地东缘大宁-吉县区块为例

深部煤储层孔隙–裂缝结构对深部煤层气资源潜力评价和勘探开发具有重要意义。选取鄂尔多斯盆地东缘大宁–吉县区块DJ57井本溪组5个煤岩样品为研究对象,在煤岩煤质参数测试的基础上,采用气体吸附法、高压压汞法和微米CT扫描等测试手段,对深部煤储层中的纳米级孔隙-微米级裂缝进行多尺度定量表征,综合评价不同尺度的孔裂隙结构特征。再结合渗透率和甲烷等温吸附试验,探讨了微观孔裂隙对深部煤储层中煤层气的赋存和渗流的影响。研究结果表明:基于多种孔隙表征方法对深部煤储层孔裂隙进行多尺度定量表征,其孔裂隙体积分布类型主要以“U”型为主,呈现出微孔与微裂缝并存双峰态,主要集中在0.3~1.5 nm和>100μm的范围内。其中,微孔(<2 nm)、介孔(2~50 nm)、宏孔(50 nm~10μm)和微裂缝(>10μm)体积平均分别占总孔裂隙体积的80.18%,6.70%,1.65%和11.47%。随着微孔发育而吸附气量呈增大的趋势,微孔可以提供大量吸附点位,为深部煤层气的吸附和赋存提供场所。随着微裂缝发育而游离气量呈增大的趋势,微裂缝可以提供大量储集空间,为深部煤层气的富集提供空间条件。此外,微裂缝在三维空间中相互连通,形成网状结构,连通性强。随着微裂缝越发育,煤储层渗透率越大,微裂缝增强了煤层气的渗流能力。纳米级孔隙和微米级裂隙发育特征分别控制着深部煤层气吸附能力和开发潜力。

四川盆地“槽-隆”控制下的寒武系筇竹寺组页岩储层特征及其差异性成因

四川盆地寒武系筇竹寺组是继五峰组-龙马溪组后页岩气勘探开发的重要接替层位,目前在德阳-安岳裂陷槽中心和槽缘部署的Z201井和WY1井页岩气勘探取得良好效果,但裂陷槽内筇竹寺组页岩储层发育特征仍不清楚。以槽内中心Z201井和槽缘WY1井为重点,结合其他页岩气勘探开发资料,系统分析了研究区筇竹寺组页岩各小层矿物特征、有机地化特征、储层及储集空间特征、含气性特征。研究结果表明:①筇竹寺组可划分为8个小层,页岩整体以脆性矿物为主,总有机碳含量(TOC)普遍大于1%,为优质烃源岩,且槽内TOC高于槽缘,具备良好的生气条件。②筇竹寺组页岩有机孔与无机孔均发育,槽内孔隙发育更好,具有极高的含气量。1,3,5和7小层黑色页岩储层品质较好,5小层储层品质最优。③德阳-安岳裂陷槽控制了筇竹寺组页岩储层发育,槽内Z201井钻遇的筇竹寺组页岩储层优于槽缘WY1井。④乐山-龙女寺古隆起控制筇竹寺组页岩有机质演化程度,古隆起内筇竹寺组有机质热演化成熟度普遍低于古隆起外,隆起区适中的热演化程度具备大规模富气的条件。筇竹寺组页岩储层各项条件较好,是未来页岩气勘探开发的主要接替区域。

二氧化碳-水-岩作用机理及微观模拟方法研究进展

系统综述CO_(2)-水-岩复杂作用机理、多孔介质反应输运(溶解、沉淀及沉淀运移)微观模拟、CO_(2)-水-岩系统微观模拟3个方面的研究进展,指出目前研究存在的主要问题并提出了关于未来研究方向的建议。CO_(2)注入储集层后,不仅存在常规渗流体系的流动和传质作用,还会产生溶解、沉淀及沉淀运移等特殊物理化学现象,其耦合作用导致多孔介质的孔渗参数变化规律复杂。孔隙尺度的微观渗流模拟,可以得到孔喉三维空间内的详细信息,且能显性观察到多孔介质流-固界面随反应的变化。目前研究主要在复杂作用机理解耦合、多矿物差异性反应表征、沉淀生成机理及表征(晶体成核和矿物脱落)、沉淀-流体相互作用模拟方法、多物理化学过程耦合渗流机制等方面存在局限。未来研究中,需要创新实验方法对“溶解—沉淀—沉淀运移”解耦合,提高矿物地球化学反应相关参数实验测试的准确度,在不同沉淀机理可靠表征的基础上,建立沉淀-流体相互作用模拟方法,并有机耦合各个物理化学过程,最终实现对CO_(2)-水-岩系统中“溶解—沉淀—沉淀运移”的耦合渗流模拟。

水资源-能源-粮食-生态系统耦合协调及驱动力分析

为加深对我国水资源、能源、粮食、生态系统协同演变趋势的认识,构建水资源-能源-粮食-生态多维系统指标体系,运用耦合协调度模型对我国2005—2020年水资源-能源-粮食-生态系统耦合协调度进行评价,并采用多因素归因分析法进行驱动力分析。结果表明:我国水资源-能源-粮食-生态系统耦合协调度从2005年的0.55增长到2020年的0.84,各地区耦合协调度从勉强协调发展水平过渡到中级协调发展水平,各子系统对耦合协调度上升的驱动分别经历了由粮食子系统到生态子系统再到水资源子系统主导的过程;能源子系统的贡献率虽然比较小,但是未来可能是各地区提升水资源-能源-粮食-生态系统多维系统协调发展水平的突破口。

基于UPLC-QTOF-MS解析苦荞黄酮组成及药理学网络分析

为优化苦荞黄酮提取工艺并明确其具体成分结构和含量及药理作用,本研究以四川省凉山彝族自治州甘洛县优质苦荞为研究对象,对超声提取苦荞黄酮工艺进行了优化,采用超高效液相色谱-四级杆-飞行时间质谱(UPLC-QTOF-MS)对主要黄酮成分进行结构鉴定,并采用超高效液相色谱-三重四级杆质谱联用仪对鉴定到的黄酮进行准确定量,同时利用中药系统药理学(TCMSP)系统分析其网络药理学特性。结果表明,超声辅助乙醇提取苦荞黄酮的最优条件为乙醇浓度90%(V/V)、超声功率140 W、超声温度70℃、超声时间60 min、提取溶剂与苦荞原料比50∶1(mL·g^(-1)),该条件下,提取液中共鉴定到黄酮16种,其中芦丁、表儿茶素和儿茶素含量分别达到115.81、72.99和23.08μg·mL^(-1)。这16种黄酮在防治心血管疾病、慢性炎症性疾病上具有重要作用。本研究可为苦荞精深加工综合利用尤其是功能性苦荞产品开发利用奠定基础。

基于“心-脉-神”互言探讨肝心同治冠心病合并抑郁(双心疾病)的理论研究

双心疾病作为“血脉之心”与“神明之心”同病的复合疾病,已经成为现代社会影响人类健康的主流问题之一,其中的冠心病合并抑郁属于临床中常见的发病类型。冠心病是一种严重威胁健康的心血管疾病,焦虑和抑郁是其不良预后的潜在危险因素。冠心病合并抑郁属中医“胸痹”“郁证”范畴,“心藏脉,脉舍神”,心脏对生命活动具有重要的控制和调节作用,“从心论治”使机体心主神明、心主血脉功能正常发挥。心血管疾病与情志病是密不可分的,胸痹患者心脉不畅,肝失疏泄,痰瘀互结,气机郁滞加重,由此引发情志的改变。双心疾病与中医的“心主血脉”“心主神明”“肝主藏血”“肝主疏泄”功能失常密切相关,“心”与“肝”的状态失衡是导致疾病进展的主要因素,故“肝心同治”是调节关键病机-肝心失调的必由之法,以疏肝解郁、调气和血为主。基于对“从心论治”“心-脉-神”与“肝心同治”的理论探讨,结合现代科学技术,旨在为防治冠心病合并抑郁提供新的思路与机制预测。

高速铁路主跨320 m钢-混部分斜拉桥无砟轨道适应性研究

南玉高铁六景郁江特大桥设计将钢-混部分斜拉桥结构引入时速350 km高速铁路领域,而300 m级以上大跨度桥上无砟轨道的竖向变形极易超限,影响列车通过的安全性和舒适性,因此,系统研究在此大跨桥梁结构上铺设无砟轨道的适应性十分必要。通过建立有限元及动力学模型,分析不同组合工况下无砟轨道结构的变形特点及动力特性,运用60 m弦测法探究各工况下无砟轨道的线形变化规律,从而确定大跨度钢-混部分斜拉桥铺设无砟轨道的适应性,并对设计和施工提出合理化建议。主要结论如下:在各种不利组合荷载作用下,桥上无砟轨道结构强度满足规范要求,列车通过大桥的各项安全性与舒适性指标均满足规范要求;混凝土收缩徐变和斜拉索升降温是影响无砟轨道线形标准的两大主因,应在无砟轨道施工前确保足够的沉降观测期和收缩徐变释放期,并充分考虑拉索的保温设计;在温度组合荷载作用下,桥上无砟轨道的60 m弦测不平顺幅值为6.79 mm,满足高速铁路静态验收标准;但在叠加列车荷载和收缩徐变后,变形弦测值均出现Ⅱ级及以上超限,通过合理设置预拱度后可有效改善轨道平顺性标准。

老年急性脑梗死患者血清Del-1和IL-17水平变化及与梗死面积和预后的关系

目的 探究老年急性脑梗死(ACI)患者血清内皮发育调节基因-1(Del-1)、白细胞介素-17(IL-17)水平与脑梗死面积、病情严重程度及预后的关系。方法 回顾性收集2019-01-2021-12厦门大学附属东南医院收治的126例老年ACI患者(病例组)及105名健康体检者(对照组)的临床资料,根据脑梗死面积将病例组患者分为大面积梗死组(梗死最大直径>5 cm,n=14)、中面积梗死组(梗死最大直径3~5 cm,n=53)和小面积梗死组(梗死最大直径<3 cm,n=59);根据NIHSS评分分为重症组(NIHSS评分≥16分,n=13)、中症组(5分<NIHSS评分<15分,n=58)和轻症组(NIHSS评分≤5分,n=55);根据m RS评分分为预后良好组(mRS评分≤2分,n=81)和预后不良组(mRS评分>2分,n=45)。采用荧光免疫法检测血清Del-1、IL-17水平,受试者工作特征(ROC)曲线评估血清Del-1、IL-17水平预测老年ACI患者预后的价值。结果 病例组吸烟史比例、收缩压、舒张压、糖化血红蛋白、血清IL-17水平均高于对照组,血清Del-1水平低于对照组(P<0.05)。不同脑梗死面积患者血清Del-1水平比较,小面积梗死组>中面积梗死组>大面积梗死组;血清IL-17水平比较,小面积梗死组<中面积梗死组<大面积梗死组(P<0.05)。轻症组血清Del-1水平高于中症组、重症组(P<0.05),不同病情严重程度患者血清IL-17水平比较,重症组>中症组>轻症组(P<0.05)。预后良好组患者血清Del-1水平高于预后不良组,血清IL-17水平低于预后不良组(P<0.05)。ROC曲线分析显示,血清Del-1、IL-17预测ACI患者预后的AUC值分别为0.763、0.747(P<0.05)。结论 老年ACI患者血清Del-1水平较低,IL-17水平较高,二者与患者脑梗死面积、病情严重程度和预后关系密切,可作为预测老年ACI患者预后的可靠指标。

基于DEMATEL-ISM的水利工程EPC项目价值增值机理研究

采用设计-采购-施工(engineering-procurement-construction,EPC)总承包模式的水利工程项目日益增多,研究其价值增值机理有利于总承包方做好项目的价值管理。从水利工程EPC项目的价值链分析入手,基于文献和专家访谈得到23个价值增值影响因素。采用问卷调查方式得到各因素间的影响程度评分,用决策实验和评估实验(decision-making trial and evaluation laboratory,DEMATEL)法计算了各因素的中心度和原因度,结合解释结构模型(interpretative structural modeling,ISM)对数据进行分析,将价值增值因素划分为6类,构建了水利工程EPC项目价值增值的递阶模型,探究和揭示了项目价值增值的路径和机理。研究结果对水利工程EPC总承包方制订管理策略有一定启示作用。

基于混合式教学的“教-学-评”一体化实验教学体系探索

实验能力是医学专业研究生的重要科研能力,实验能力的培养与实验教学的方法与质量密切相关。文章针对传统实验教学受到时间和空间限制且评价指标较为单一的现状,提出构建基于线上自主学习和现场实践相结合的“教-学-评”一体化实验教学体系,建立覆盖课前线上自主学习、课堂现场实践、课后作业提交与考核教学全过程的评价体系,以评促学,以评促教,通过评价反馈激发学生的学习热情,改进教学内容和方法,不断探索与完善实验教学体系,提高实验教学质量,以期为培养具有实践能力与创新精神的医学科研人才发挥积极作用。

东昆仑大格勒地区碱性岩-碳酸岩型铌矿勘查进展及找矿前景

铌广泛应用在冶金工业、原子能工业、航空航天工业、军事工业、电子工业、超导材料及医疗仪器等方面,是全球高度关注的关键矿产。碱性岩-碳酸岩型矿床赋存了世界上大部分的铌资源,而我国铌资源禀赋差,对外依存度大于90%。2021年青海省地质调查院在东昆仑大格勒地区发现了碱性岩-碳酸岩型铌矿,通过三年的勘查工作,圈定5条铌矿体,矿体延伸长160~1280 m,控制最大斜深800 m,矿体厚度4.3~115.7 m,Nb_(2)O_(5)平均品位0.092%~0.156%,伴生P_(2)O_(5)平均品位3.8%~5.6%。通过资源量估算,Nb_(2)O_(5)推断资源量超过10万吨,已达大型矿床规模。目前铌矿体在走向和倾向上延伸稳定,显示出良好的找矿前景。

健脾益肠散对溃疡性结肠炎大鼠NLRP3信号通路IL-1β、IL-18表达的影响

目的探讨健脾益肠散对溃疡性结肠炎(UC)模型大鼠NLRP3信号通路白细胞介素(IL)-1β、IL-18表达的影响。方法从40只SD大鼠随机选取10只作为正常组,其余大鼠自由饮用5%硫酸葡聚糖溶液7 d制备UC大鼠模型,将成模大鼠随机分为模型组、柳氮磺吡啶组和健脾益肠散组,每组10只。健脾益肠散组和柳氮磺吡啶组予相应药液灌胃,正常组和模型组予等体积蒸馏水灌胃,连续14 d。观察大鼠一般状况,并进行疾病活动指数(DAI)评分,ELISA检测大鼠血清核苷酸结合寡聚化结构域样受体蛋白3(NLRP3)、凋亡相关斑点样蛋白(ASC)、胱天蛋白酶1(Caspase-l)含量,免疫组化染色、Western blot和RT-PCR检测结肠组织IL-1β、IL-18蛋白及mRNA表达。结果与正常组比较,模型组大鼠一般状况较差,DAI评分显著升高(P<0.01),血清NLRP3、ASC、Caspase-l含量显著增加(P<0.01),结肠组织IL-1β、IL-18蛋白和mRNA表达均显著升高(P<0.01);与模型组比较,健脾益肠散组和柳氮磺嘧啶组大鼠一般状况明显好转,DAI评分显著降低(P<0.01),血清NLRP3、ASC、Caspase-l含量明显减少(P<0.05,P<0.01),结肠组织IL-1β、IL-18蛋白和mRNA表达均明显降低(P<0.05,P<0.01)。结论健脾益肠散可抑制NLRP3信号通路IL-1β、IL-18表达,改善结肠免疫炎症损伤,发挥治疗UC作用。

蒙药协日嘎-4汤对糖尿病肾病大鼠肾保护作用及肾组织单核细胞趋化蛋白-1表达

目的 探讨蒙药协日嘎-4汤对糖尿病肾病(DN)大鼠肾保护作用及可能的作用机制。方法 60只Wistar大鼠随机分为正常对照组、模型组、阳性对照组、协日嘎-4汤低、中、高剂量组等6组,每组10只。治疗8 w后观察各组24 h尿蛋白定量、血清尿素氮(BUN)、血肌酐(Scr)、肿瘤坏死因子(TNF)-α、白细胞介素(IL)-6、C反应蛋白(CRP)及肾组织病理变化和单核细胞趋化(MCP)-1表达。结果 与模型组比较,阳性对照组和协日嘎-4汤低、中、高剂量组血清BUN、Scr、TNF-α、IL-6、CRP水平和24 h尿蛋白定量均明显降低(P<0.05),协日嘎-4汤高剂量组更显著(P<0.01);各治疗组肾小管空泡变性、肾小球基底膜增厚及系膜增生改变明显减轻;肾组织MCP-1表达不同程度明显减少(P<0.05),协日嘎-4汤高剂量组更显著(P<0.01)。结论 蒙药协日嘎-4汤可通过下调DN大鼠肾组织MCP-1表达、降低炎症因子分泌,从而发挥肾脏保护作用。

新风胶囊抑制软骨细胞炎症和细胞外基质降解:基于调控miR-502-5p/TRAF2/NF-κB轴

目的探讨新风胶囊(XFC)对白介素(IL)-1β诱导的软骨细胞功能的影响及作用机制。方法构建IL-1β诱导的软骨细胞炎症模型;SD大鼠灌胃制备XFC含药血清。细胞增殖实验(CCK-8)和流式细胞术筛选最佳XFC含药血清浓度;双荧光素酶报告分析miR-502-5p和TRAF2的靶向关系。构建miR-502-5p抑制表达质粒(inhibitor)及阴性对照组,转染至软骨细胞中。分为对照组(NC),IL-1β组,XFC组,IL-1β+NC-inhibitor,IL-1β+miR-502-5pinhibitor,IL-1β+miR-502-5pinhibitor+XFC最佳含药血清组,酶联免疫吸附试验(ELASA)检测IL-1β、肿瘤坏死因子-α(TNF-α)、IL-4、IL-10的水平。逆转录PCR(RT-PCR)、蛋白质免疫印迹实验(WB)、免疫荧光法检测Ⅱ型胶原α1(COL2A1)、基质金属蛋白酶13(MMP13)、软骨蛋白聚糖抗体(ADAMTS5)和miR-502-5p/TRAF2/NF-κB基因的表达。结果与NC组相比,IL-1β组中软骨细胞活力下降,细胞凋亡率升高,且miR-502-5p、IL-4、IL-10和COL2A1表达下降,IL-1β、TNF-α和ADAMTS5、MMP13、TRAF2、NF-κB p65表达升高(P<0.05)。筛选得出20%XFC为最佳含药血清浓度。与IL-1β组相比,XFC含药血清干预后,软骨细胞活力升高,细胞凋亡率下降,IL-1β、TNF-α、ADAMTS5、MMP13、TRAF2、NF-κBp65表达下降,miR-502-5p、IL-4、IL-10和COL2A1表达升高(P<0.05)。与NC-inhibitor相比,转染miR-502-5p inhibitor后,IL-1β、TNF-α、ADAMTS5、MMP13、TRAF2、NF-κB p65表达升高,miR-502-5p、IL-4、IL-10和COL2A1表达下降;与miR-502-5pinhibitor相比,将miR-502-5pinhibitor转染的软骨细胞和最佳XFC含药血清共培养后,XFC含药血清能逆转miR-502-5p抑制状态对软骨细胞炎症和ECM的影响。结论XFC抑制软骨细胞炎症、细胞外基质降解,减轻IL-1β诱导的软骨细胞损伤,其机制可能是通过调节miR-502-5p/TRAF2/NF-κB轴。