以钙钛矿型复合氧化物为前驱体构筑La-Ce氧化物修饰的Pt-Co纳米双金属催化剂及其对CO氧化的性能

利用钙钛矿型复合氧化物(PTO)可以将多种金属离子限域并均匀混合于钙钛矿晶格中的特点,提出了一种构筑氧化物修饰的纳米双金属催化剂团簇的新构想。以担载于大比表面积SiO 2上的钙钛矿型复合氧化物La1-y Cey Co0.87 Pt0.13 O3/SiO 2作为前驱体,将La、Ce、Co和Pt多种金属离子均匀混合并限域于PTO晶粒中,还原后得到Pt-Co/La-Ce-O/SiO 2催化剂;通过氮气吸附-脱附、XRD、H2-TPR和TEM等手段对Pt-Co/La-Ce-O/SiO 2催化剂进行了表征,考察了其对CO氧化的催化性能,研究了构效关系。结果发现,La-Ce-O-Pt-Co构成了纳米团簇,担载于SiO2表面,形成了Pt-Co纳米双金属颗粒;Co修饰Pt提高了其催化活性,而添加Ce进一步改善了其催化性能。当Ce含量(y)为0.2时,催化剂La0.8 Ce0.2 Co0.87 Pt0.13 O3/SiO2的活性最佳,在120℃下即可实现CO完全转化,且在含体积分数15%H 2O及12.5%CO 2的气氛中仍具有较好的催化性能。稳定性测试表明,所制得的Pt-Co/La-Ce-O/SiO 2催化剂具有良好的稳定性和抗烧结性能。

氧化应激、炎症和自噬在脑缺血损伤中作用机制及治疗策略

脑缺血是世界范围内导致人类致残致死的主要疾病,目前尚缺乏有效的治疗措施。近期大量研究证据表明,氧化应激、炎症和自噬是脑缺血损伤病理过程中的关键分子事件,且三者之间存在密切和复杂的相互作用。本文对脑缺血损伤中三者的调节机制及其相互作用研究进展进行综述,在此基础上,进一步讨论脑缺血损伤的潜在治疗干预措施,为寻找有效的神经保护策略提供新思路。

神经炎症和自噬在脑损伤中的作用

神经炎症反应在脑损伤的发病机制中起重要作用。自噬是降解细胞内机能障碍的蛋白质和损伤的细胞器的关键生物学过程。自噬异常通过影响炎症反应参与中枢疾病的发病过程。本文对炎症和自噬参与脑损伤病理过程的研究进展进行综述,并进一步讨论自噬对炎症反应的调节机制。

基于Endo-M N175Q糖链转移反应与丙酮富集糖肽的LC-MS分析糖蛋白N-糖链

基于化学酶标记和丙酮富集糖肽方法,建立了一种可靠、有效、简单的糖蛋白N-糖链分析方法。以唾液酸糖肽(SGP)为模型糖肽,比较了样品中丙酮加入量对SGP的富集效果,最终选择加入样品体积5倍量的丙酮。用丙酮富集经胰蛋白处理的核糖核酸酶B(RNase B)酶解液中的糖肽,以富集分离得到的糖肽(糖基供体)和PDPZ-Boc-Asn-GlcNAc(糖基受体)作为酶反应底物,进行Endo-M N175Q的转糖基反应,得到PDPZBoc-Asn-GlcNAc-N-糖链标记物。采用YMC C18色谱柱为分析柱,10 mmol/L甲酸铵-乙腈为流动相梯度洗脱,经液相色谱-串联质谱(LC-MS)检测得到5种高甘露糖型糖链。结果表明,丙酮可有效地富集大量肽和少量糖肽混合溶液中的糖肽,Endo-M N175Q可将天然糖肽的糖链转移到PDPZ-Boc-Asn-GlcNAc受体上。将该方法应用于胎球蛋白N-糖链分析,检测到5种复杂型N-糖链。该研究为各种糖蛋白N-糖链检测提供了新的分析方法。

CuO修饰的Cu_(1.5)Mn_(1.5)O_(4)尖晶石型复合氧化物对CO氧化的协同催化

铜锰复合氧化物是常用的氧化反应催化剂,一般认为铜锰尖晶石是活性组分;同时氧化铜和氧化锰也具有催化活性,但性能较差。研究表明,发现Cu_(1.5)Mn_(1.5)O_(4)和CuO的协同效应能促进CO的催化氧化。催化剂以柠檬酸络合法制备,采用氮气吸附-脱附、XRD、H_(2)-TPR、TEM、CO-TPD和O_(2)-TPD等手段对系列催化剂进行了表征,测试了对CO氧化的催化性能。结果表明,CuO修饰的Cu_(1.5)Mn_(1.5)O_(4)具有最好的催化性能和最高的单位表面活性(以单位表面积CO转化率计),表明CuO与Cu_(1.5)Mn_(1.5)O_(4)存在协同作用。认为协同作用源自CuO活化的O_(2)和Cu_(1.5)Mn_(1.5)O_(4)活化的CO结合生成CO_(2)提高了活性。

小胶质细胞激活研究中免疫组化和荧光技术的应用

目的在体内和体外实验中应用免疫组化(immunohistochemistry, IHC)和免疫荧光(immunofluorescence, IF)技术检测神经炎症过程中小胶质细胞激活及炎症分子表达改变。方法应用IHC方法观察脂多糖(lipopolysaccharide,LPS)诱导SD大鼠脑内小胶质细胞离子钙接头蛋白分子1(ionized calciumbinding adaptor molecule 1, Iba-1)免疫标记的小胶质细胞改变;应用IF方法检测LPS诱导体外培养的小鼠小胶质细胞系BV2细胞吞噬异硫氰酸荧光素(fluorescein isothiocyanate, FITC)标记的荧光微球活性以及炎症细胞因子白细胞介素1 beta(interleukin 1beta, IL1beta)的表达变化。结果 IHC结果显示,2.5 mg/kg LPS可诱导大鼠皮层Iba-1阳性小胶质细胞形态改变;IF结果显示,10 ng/mL LPS组和100 ng/mL LPS组BV2细胞荧光微球吞噬率与对照组比较,差异均有统计学意义(P<0.05);100 ng/mL LPS处理后,BV2细胞的炎症细胞因子IL1beta表达上调。结论应用IHC和IF技术可证实LPS模型中小胶质细胞激活及炎症细胞分子表达改变。

5-Lipoxygenase and cysteinyl leukotriene receptors in neuroinflammation and neuronal injury

Brian ischemic injury and central neurodegenerative diseases as leading contributors to disability and death have become a majorclinical and public health concern worldwide.Neuroinflammation plays a pivotal role in the pathological progression of cerebral ischemia and neurodegenerative diseases including Parkinson disease(PD).Therefore,it is important to find effective therapeutic targets to attenuate inflammation and delay the progression of brain injury.Cysteinyl leukotrienes(CysLTs) are potent inflammatory mediators synthesized from arachidonic acid by 5-lipoxygenase(5-LOX) in the central nervous system.Two distinct G-protein-coupled receptors,CysLT1 R and CysLT2 R,mediate most of the known CysLTs biological responses.Accumulating evidence has demonstrated that postischemic inflammation and neuronal loss are mediated by 5-LOX and CysLTRs fol owing focal cerebral ischemia.We recently reported that the expression of 5-LOX,CysLT1R and inflammatory vascular cell adhesion molecule-1(VCAM-1) was upregulated in the hippocampus of rats with transient global cerebral ischemia,which was closely associated with delayed neuronal death in the hippocampal CA1 area.5-LOX inhibitor zileuton,CysLT1R antagonist ONO-1078 and montelukast dose-dependently reduced hippocampal CA1 neuronal death and inhibited the increased expression of 5-LOX and VCAM-1.In vitro ischemia-like injury in 5-LOXtransfected PC12 cells,oxygen-glucose deprivation(OGD) induced cell death mediated by5-LOX via ROS/P38 MAPK pathway.The nonselective 5-LOX inhibitor caffeic acid inhibited OGDstimulated activation of 5-LOX and ROS/P38 MAPK signaling and improved neuronal survival.In PD model,high concentrations of rotenone caused directly PC12 neurotoxicity,which was modulated by 5-LOX and abolished by suppression of 5-LOX.It is well known that microglia is major modulators of inflammatory response after brain injury.Overactivated microglia and production of proinflammatory cytokine IL-1β,IL-6 and TNF-α contribute to the neuroinflammation and brain injury.5-LOX,CysLT1R and CysLT2R are involved in microglial activation and resultant neurotoxic responses.It has been found that low concentrations of rotenone can activate 5-LOX and CysLT1R on microglial cells to enhance microglial inflammation and microglia-dependent neuronal death in vitro.5-LOX inhibitor zileuton and CysLT1R antagonist montelukast protected neurons from microglia-dependent rotenone neurotoxicity.Furthermore,lipopolysaccharide(LPS)induced microglial activation and microglial neurotoxicity mediated by CysLT2R in vitro.Both pharmacological blockade(CysLT2R antagonist HAMI3379) and RNA interference(specific short hairpin RNA) of CysLT2 R significantly attenuated LPS-triggered microglial inflammation and subsequent neuronal death.Collectively,the present results indicate the role of 5-LOX and CysLTRs in neuroinflammation and brain injury.Modulation of 5-LOX and CysLTRs may be potential therapeutic approaches for inflammation-related brain disorders such as cerebral ischemia and PD.However,further research is needed to clarify the mechanisms underlying the regulation of neuinflammatory processes by 5-LOX and CysLTRs.

二维斑点追踪成像技术评估无心肌梗死冠心病三支血管病变患者的右心室功能的临床应用价值

目的:利用二维斑点追踪成像技术(2D-STE)评价有冠心病三支血管病变但不合并心肌梗死的病人右心室功能初期变化。方法:随机采集30例行健康检查的体检者设为对照组(A组)。另选取本院已行冠状动脉造影且结果显示为冠状动脉三支血管发生病变的患者60例,根据其三支血管的狭窄程度分为两组,32例狭窄率为50%~<75%划入B组。28例狭窄率≥75%划入C组。收集患者一般资料;常规超声得到三尖瓣环平面收缩位移(TAPSE)、收缩期峰值速度(s’)、舒张早期和舒张晚期峰值速度(e’,a’)、右心室收缩末期、舒张末期容积(RVESV、RVEDV)计算得到右室射血分数(RVEF);利用2D-STE获得右室收缩期整体应变(GS)、收缩期、舒张早晚期应变率(SRs、SRe、SRa)。利用Pearson线性相关,分析受检者GS和N末端B型脑钠肽前体(NT-pro BNP)及之间的相关性。结果:与A组相比,B组e’、e’/a’减小(P<0.05),而s’、E/A、FAC、TAPSE、LVEF及RVEF无明显统计学差异(均P>0.05);与A、B两组相比,C组RVEF、LVEF、E/A、e’、e’/a’、s’、FAC及TAPSE均减低(均P<0.05)。2D-STE参数:与A组相比,B、C两组GS、SRe、SRa、S、SRs均减低,且C组各参数较B组降低更明显(均P<0.05);相关性分析显示B、C组GS与血清NT-pro BNP有较强的负相关关联性(r=-0.91,r=-0.64,P<0.05)。结论:2D-STE是评估无心肌梗死型冠心病三支血管病变患者的右心室早期功能改变的可行方法。