孟鲁司特治疗儿童支气管哮喘急性发作期的疗效及对循环CD4^+CD25^+调节性T细胞表达的影响

目的研究孟鲁司特对支气管哮喘急性发作期患儿外周血中CD4+CD25+调节性T细胞(Tregs)表达的影响及临床疗效。方法选取94例急性发作期的支气管哮喘患儿为研究对象,按随机数字表法将患儿分为对照组与观察组,每组47例。给予对照组患儿布地奈德混悬液0.5 mg/2 mL雾化吸入治疗,1次/d,连续治疗4周;观察组在此基础上加用孟鲁司特钠咀嚼片5 mg,1次/d,睡前口服,连用4周。酶联免疫吸附法(ELISA)检测患儿血清γ干扰素(IFN-γ)及血清白细胞介素-5(IL-5)水平,并进行日间、夜间症状评分,评价肺功能。采用流式细胞术分别对治疗前后患儿外周血中CD4+CD25+Tregs的表达水平进行检测。结果与治疗前相比,治疗后患儿的各项肺功能指标均改善良好,且相比于对照组,观察组的变化更显著,差异有统计学意义(P<0.05);在日间、夜间症状评分方面,与治疗前相比,两组患儿分数均呈下降趋势且观察组下降显著(P<0.05);治疗后患儿的IL-5水平均明显降低,IFN-γ水平均明显升高,且观察组变化程度更大(P<0.05);在CD4+CD25+Tregs表达方面,治疗后其表达水平均有所提高,观察组提高程度更大(P<0.05)。结论孟鲁司特能改善患儿肺功能及患儿哮喘日间、夜间症状评分,并通过上调CD4+CD25+Tregs比例,进而分泌表达IFN-γ、IL-5,达到抑制哮喘炎症反应的效果,是治疗治疗儿童急性支气管哮喘的有效药物。

复吹转炉渣金间传质物理模拟及应用

将200t复吹转炉按照1∶12的比例缩小,用液体石蜡模拟炉渣、水模拟钢水、压缩空气模拟顶吹和底吹气体,在实验室建立模拟复吹转炉吹炼过程熔池渣金间传质的试验模型,在顶吹气体流量为88m^(3)/h条件下,通过相对集中非对称布置的4、6、8、10、12支底枪吹入不同底吹气体,用苯甲酸作为传输物质,试验测定了复吹转炉熔池渣金间的容量传质系数,考察不同底枪支数和布置以及底吹气体流量对渣金间传质速率的影响,优化复吹转炉底枪布置和底吹气体流量,以增强复吹转炉熔池的搅拌,改善熔池渣金反应动力学条件。研究结果表明,当底吹气体流量为1.14m^(3)/h时,在4~12支的底枪布置方案中,4、6支底枪布置方案的容量传质系数(分别为1.77×10^(-4)、1.80×10^(-4)L/s)低于8、10、12支底枪布置方案的容量传质系数(分别为2.41×10^(-4)、2.24×10^(-4)、2.42×10^(-4)L/s);当底吹气体流量为0.57m^(3)/h时,在8~12支底枪布置方案中,10、12支底枪布置方案的容量传质系数(分别为1.68×10^(-4)、1.69×10^(-4)L/s)明显大于8支底枪布置方案的容量传质系数(0.95×10^(-4)L/s);在底吹气体流量不小于1.14m^(3)/h后,8、10、12支底枪布置的容量传质系数相差不大,在2.24×10^(-4)~2.87×10^(-4)L/s的范围;在气体流量小于1.14m^(3)/h时,随着底吹气体流量的增加,渣金间的容量传质系数增加显著,底吹气体流量大于1.14 m^(3)/h后,容量传质系数增加变缓。将12支底枪布置方案应用到实际复吹转炉,整个炉役的平均碳氧积为0.00196×10^(-4),在不同炉龄阶段,终点钢水平均碳氧积为0.00188×10^(-4)~0.00204×10^(-4),终点钢水碳氧积小于0.0025×10^(-4)的炉次比例达到90.53%。

复吹转炉底吹非均匀供气对熔池搅拌混匀的影响

为了强化转炉熔池的搅拌,在200 t复吹转炉1∶12的模型进行物理模拟试验,研究了底吹非均匀供气对转炉复吹和纯底吹熔池的搅拌混匀效果;采用数学模拟的方法计算了纯底吹条件下,转炉采用底吹非均匀供气时的熔池流体流动。研究结果表明,在所研究的不同的底吹非均匀供气方案中,与底吹均匀供气方案相比,线性底吹非均匀供气方案有利于改善转炉熔池搅拌效果,最佳的底吹非均匀供气方案的混匀时间比均匀供气降低了19%~25%。复吹时底吹非均匀供气的混匀时间降低程度要比纯底吹的非均匀供气大,即复吹条件下,底吹采用非均匀供气更有利于熔池搅拌混匀。采用线性底吹非均匀供气方案时,在熔池内形成了明显的大循环非对称流动,有利于整个熔池内的对流传质,从而缩短了混匀时间。

The Zuo Jin Wan Formula increases chemosensitivity of human primary gastric cancer cells by AKT mediated mitochondrial translocation of cofilin-1

Resistance to cisplatin(DDP)-based chemotherapy is a major cause of treatment failure in human gastric cancer(GC). It is necessary to identify the drugs to re-sensitize GC cells to DDP. In our previous research, Zuo Jin Wan Formula(ZJW) has been proved could increase the mitochondrial apoptosis via cofilin-1 in a immortalized cell line, SGC-7901/DDP. Due to the immortalized cells may still difficult highly recapitulate the important molecular events in vivo, primary GC cells model derived from clinical patient was constructed in the present study to further evaluate the effect of ZJW and the underlying molecular mechanism. Immunofluorescent staining was used to indentify primary cultured human GC cells. Western blotting was carried out to detect the protein expression. Cell Counting Kit-8(CCK-8) was used to evaluate cell proliferation. Flow cytometry analysis was performed to assess cell apoptosis. ZJW inhibited proliferation and induced apoptosis in primary DDP-resistant GC cells. Notably, the apoptosis in GC cells was mediated by inducing cofilin-1 mitochondrial translocation, down-regulating Bcl-2 and up-regulating Bax expression. Surprisingly, the level of p-AKT protein was higher in DDP-resistant GC cells than that of the DDP-sensitive GC cells, and the activation of AKT could attenuate ZJW-induced sensitivity to DDP. These data revealed that ZJW can increase the chemosensitivity in DDP-resistant primary GC cells by inducing mitochondrial apoptosis and AKT inactivation. The combining chemotherapy with ZJW may be an effective therapeutic strategy for GC chemoresistance patients.