单钯型汽车尾气净化催化剂研究

应用流动体系微型反应和怠速实验装置对Pd/Ni/La-Ce-Al汽车尾气净化催化剂的CO、C3H8、NO转化活性进行了评价、研究了镍含量和La-Ce-Al涂层对催化剂活性的影响、对催化剂进行了TPR、CO-TPD、O2-TPD、C3H8-TPD表征.结果表明:镍对Pd/La-Ce-Al催化剂具有良好的助催化作用;在实验条件下,镍含量为15%时催化剂小试评价具有最好的CO、C3H8氧化活性和NO还原活性;La-Ce-Al涂层比例对催化剂转化活性影响很大;Pd/Ni/La-Ce-Al催化剂具有非常高的CO、HC三效氧化活性,但其NO三效还原活性有待改善.     

稀土-过渡金属复合氧化物催化剂用于汽车尾气净化研究

以不含贵金属的稀土 过渡族金属四元复合氧化物为催化剂 ,模拟汽车尾气的组成含量 ,运用连续流动式反应器 ,研究了四元复合氧化物La0 5Sr0 5Ni1 -xCuxO3系列 (x =0—1 0 )对CO和NOx 的催化氧化还原消除活性及其在消除反应条件的抗硫中毒能力 .实验结果表明 ,钙钛矿型四元复合氧化物催化剂La0 5Sr0 5Ni0 5Cu0 5O3对CO和NOx 的氧化还原消除都具有较高的活性 ;脉冲中毒实验指出 ,当反应温度≥ 3 0 0℃ ,SO2 在催化剂中的脉冲积累含量为 1 2 2× 1 0 - 2 mmol时 ,该复合氧化物仍表现出良好的抗硫毒性能 ,它对CO的氧化消除活性并未因体系中SO2 的存在而受到影响     

氟里昂12（CC12F2）燃烧分解催化剂性能的研究

本文对贵金属、氧化物和复合氧化物体系催化剂上氟里昂１２（Ｆ１２）燃烧分解反应进行了活性谰价和稳定性研究。结果表明：ＴｉＯ２，ＺｒＯ２／ＴｉＯ２催化剂对氟里昂１２燃烧分解反应具有良好的低温催化活性和较好的稳定性，ＺｒＯ２／ＴｉＯ２催化剂具有一定的臭氧－催化氧化活性。     

氟里昂12(CCl2F2)燃烧分解催化剂性能的研究

本文对贵金属、氧化物和复合氧化物体系催化剂上氟里昂_(12)(F_(12))燃烧分解反应进行了活性评价和稳定性研究.结果表明:TiO_2,ZrO_2/TiO_2催化剂对氟里昂_(12)燃烧分解反应具有良好的低温催化活性和较好的稳定性,ZrO_2/TiO_2催化剂具有一定的臭氧-催化氧化活性     

纳米TiO2光催化氧化异丙醇和丙酮反应的研究

分别研究了纳米TiO2 在主波长为 364nm的汞灯光照下催化氧化i C3H7OH和CH3COCH3水溶液的反应速率 .通过XRD ,TEM ,BET和FT IR PAS对催化剂进行表征 ,粉末的晶型主要为锐钛矿型 .平均粒径在 1 5nm左右 ,比表面积为 1 0 1 0± 0 2m2 ·g- 1 ,FT IR PAS的检测结果表明 ,CH3COCH3是i C3H7OH光催化氧化的中间产物 ,其光催化氧化反应为 :i C3H7OH [O]CH3COCH3[O]CH3COOH[O]…[O]CO2 H2 O     

Pd掺杂对Fe,Co系钙钛矿型三效催化剂性能的影响

用共沉淀法制备了LaFeO3，LaFe0.96Pd0.04O3，LaCoO3，LaCo0.96Pd0.04O3四种催化剂，用X－射线衍射仪（XRD）对催化剂进行了结构分析。程序升温还原（TPR）实验揭示催化剂中存在两种类型的氧种：α氧和β氧。活性评价和TPR实验表明，α氧是CO和C3H6氧化反应的活性氧种，而C3H8的氧化则由α氧和β氧共同来完成。Pd的掺杂可使ABO3中β氧的活性增强，从而使三效活性得以明显提高。     

La2O3—ZrO2缺陷萤石型燃烧催化剂的制备

缺陷萤石型Ｌａ２Ｏ３－ＺｒＯ２固溶体的催化燃烧活性受制备条件的影响，本文通过对其共沉淀前体的表面结构和热分解过程的分析，发现共沸蒸馏的办法可以有效地控制前体表面羟基的缩合过程，减少团聚，保持前体中金属离子均匀分散，为生成缺陷有序的烧结石型的Ｌａ２Ｚｒ２Ｏ７复氧化物提供了可能。复合氧化物固溶体的表面阳离子配置情况与样品的催化氧化性能密切相关，软团聚前体的烧结产物对甲烷燃烧反应具有更高的催化活性。     

铜锰钴复合氧化物催化剂对环己烷或苯深度氧化的催化活性

本文应用了研究相图与床层温差评价催化活性的方法，研究了在催化深度氧化环己烷或苯的反应中，铜、锰、钴三元氧化物催化剂体系的组成与催化活性的关系。用反应物在催化剂上起燃温度的等温图，描绘出该体系氧化物催化剂对环己烷或苯的催化氧化活性的分布。所得结果指导了用于净化苯系物废气所需催化剂的研制。     

掺碱金属对氧化锰催化剂活性影响的研究

考察了钾-锰、钠-锰、锂-锰三个系列的氧化物催化剂在不同有机物深度氧化反应中的活性变化规律,发现掺钾对氧化锰催化活性影响最显著。在丁酮、正丁醇、乙酸乙酯和丙烯腈的深度氧化反应中,掺适量钾或钠可提高氧化锰的催化活性,而在丙烯、甲烷、苯、二乙胺、吡啶和一氧化碳的深度氧化反应中,掺加碱金属则使氧化锰催化活性下降。     

σ-AgFeO2晶相对银铁复合氧化催化剂表面氧性能的影响

采用共沉淀法制备了一系列不同摩尔比的银铁复合氧化物催化剂。采用ＸＲＤ，ＴＰＤ－ＭＳ，ＴＰＲ等技术以及ＣＯ氧化反应考察银了铁复合氧化物催化剂的结构和表面氧性质。     

纳米Fe3O4对小鼠肺细胞的氧化损伤

纳米Fe3O4作为一种功能材料,在生物医药、生物靶向材料、微波吸收材料和高梯度磁分离器等方面应用前景广阔,其潜在的生物毒性也备受关注。为研究纳米Fe3O4对生物体可能造成的氧化损伤,以昆明小鼠为受试体,设置5、10、20和40mg·kg-14个染毒组,腹腔注射染毒7d后,测定小鼠肺组织中活性氧(reactive oxygen species,ROS)、还原型谷胱甘肽(glutathione,GSH)和丙二醛(malondialdehyde,MDA)的含量。结果显示,随着纳米Fe3O4染毒剂量的升高,肺组织ROS和MDA含量逐渐上升,GSH含量逐渐降低,各指标均呈一定的剂量-效应关系。剂量≥10mg·kg-1,肺组织ROS含量与对照组相比有显著差异(p<0.05);剂量≥20mg·kg-1,肺组织MDA含量与对照组相比有显著差异(p<0.05);剂量≥40mg·kg-1,肺组织GSH含量与对照组相比有显著差异(p<0.05)。研究表明,较高剂量(≥20mg·kg-1)的纳米Fe3O4颗粒材料会引起小鼠肺细胞的氧化损伤。     

Induction of apoptosis and cytokine markers in colon cancer cells by magnesium oxide (MgO) nanoparticles

Magnesium oxide nanoparticles (MgONP) are predominantly utilized in industrial products. This study was undertaken to elucidate the mechanisms underlying toxic effect of MgONP in human colon cancer (HT 29) cells over 48 hr period. Cytotoxicity was evaluated by using MTT and neutral red uptake assays. Data demonstrated that MgONP reduced cell viability in concentration- and time-dependent manner. MgONP induced oxidative stress by decreasing glutathione (GSH) concentrations and elevation of reactive oxygen species (ROS) and lipid peroxidation levels. Increased caspase-3 enzyme activity and greater condensed, damaged chromosome was observed following MgONP exposure in HT 29 cells. The level of interleukin-4 (IL-4), tumor necrosis factor (TNF-α), and DNA fragmentation were significantly higher in MgONP incubated cells. The results showed that MgONP-induced toxicity in HT 29 cells may be mediated through oxidative stress.     

Pyrite-driven reactive oxygen species formation in simulated lung fluid: implications for coal workers’ pneumoconiosis

The origin of coal worker's pneumoconiosis (CWP) has been long debated. A recent epidemiological study shows a correlation between what is essentially the concentration of pyrite within coal and the prevalence of CWP in miners. Hydrogen peroxide and hydroxyl radical, both reactive oxygen species (ROS), form as byproducts of pyrite oxidative dissolution in air-saturated water. Motivated by the possible importance of ROS in the pathogenesis of CWP, we conducted an experimental study to evaluate if ROS form as byproducts in the oxidative dissolution of pyrite in simulated lung fluid (SLF) under biologically applicable conditions and to determine the persistence of pyrite in SLF. While the rate of pyrite oxidative dissolution in SLF is suppressed by 51% when compared to that in air-saturated water, the initial amount of hydrogen peroxide formed as a byproduct in SLF is nearly doubled. Hydroxyl radical is also formed in the experiments with SLF, but at lower concentrations than in the experiments with water. The formation of these ROS indicates that the reaction mechanism for pyrite oxidative dissolution in SLF is no different from that in water. The elevated hydrogen peroxide concentration in SLF suggests that the decomposition, via the Fenton mechanism to hydroxyl radical or with Fe(III) to form water and molecular oxygen, is initially inhibited by the presence of SLF components. On the basis of the oxidative dissolution rate of pyrite measured in this paper, it is calculated that a respirable two micron pyrite particle will take over 3?years to dissolve completely.     

环境污染物导致氧化应激的关键信号通路及其检测方法

环境污染物能够以多种途径进入生物体内,在体内产生含氧自由基等活性氧物质,并通过多种信号通路及酶反应引起氧化应激,造成生物体内的脂质过氧化、蛋白质损伤、DNA表达改变、酶失活等,从而引发心血管疾病、风湿类疾病、感染及癌症等的发生。本文对环境污染物致氧化应激产生的原因、涉及的信号通路及酶反应、造成的危害,以及常见的基于细胞模型的氧化应激检测方法进行了综述,期望为评价环境污染物和检测氧化损伤提供参考。     

环境污染物导致氧化应激的关键信号通路及其检测方法

环境污染物能够以多种途径进入生物体内，在体内产生含氧自由基等活性氧物质，并通过多种信号通路及酶反应引起氧化应激，造成生物体内的脂质过氧化、蛋白质损伤、DNA表达改变、酶失活等，从而引发心血管疾病、风湿类疾病、感染及癌症等的发生。本文对环境污染物致氧化应激产生的原因、涉及的信号通路及酶反应、造成的危害，以及常见的基于细胞模型的氧化应激检测方法进行了综述，期望为评价环境污染物和检测氧化损伤提供参考。     

镉胁迫下蚯蚓金属硫蛋白氧化修饰的研究(Oxidative Modification of Metallothionein in Earthworm under Cd Stress)

金属硫蛋白(MT)是生物体内的一类富含巯基(—SH)的蛋白,在细胞氧化还原调控和重金属解毒等方面具有重要作用.MT的—SH可以络合重金属,同时对氧化作用很敏感,重金属胁迫产生的活性氧物质(ROS)可以将其氧化成二硫键(S—S).为揭示镉(Cd)对蚯蚓MT的—SH含量及其氧化修饰的影响,将蚯蚓放入Cd浓度为0、100、300mg·kg-1的黄棕壤中胁迫21天,通过SBD-F标记和高效液相色谱(HPLC)结合的方法测定MT中—SH和S—S的含量.结果显示,随着Cd浓度的增加,蚯蚓体内的—SH和S—S含量均逐渐增加,但S—S所占比例降低.这说明Cd诱导了蚯蚓体内MT合成,并且诱导量随着Cd胁迫的增强而增加,但—SH的氧化修饰程度有所下降.     

甲醛暴露时间延长加剧小鼠哮喘模型肺氧化损伤并促进IL-17表达

为了探究不同暴露时间甲醛对小鼠哮喘模型肺氧化应激及IL-17表达的影响,用浓度为3.0 mg·m~(-3)的甲醛气体吸入染毒,同时将48只雄性Balb/c小鼠随机分为6组:(1)对照组(生理盐水组);(2)ovalbumin(OVA)致敏组;(3)0.5 h甲醛+OVA组;(4)1h甲醛+OVA组;(5)1.5 h甲醛+OVA组;(6)2 h甲醛+OVA组,以不同时间长度进行甲醛暴露,连续35 d。OVA致敏组、0.5 h甲醛+OVA组、1 h甲醛+OVA组、1.5 h甲醛+OVA组、2 h甲醛+OVA组均在第11、18及25天腹腔注射OVA致敏液(5 mg OVA+175 mg Al(OH)_3+30 mL生理盐水),第29~35天(共计1周)进行1%OVA雾化(30 min·d~(-1)),每日1次,诱发哮喘。第36天进行以下操作:取肺组织测定肺系数并制作肺匀浆,检测肺组织中活性氧自由基(ROS)、丙二醛(MDA)和还原型谷胱甘肽(GSH)的含量,并采用ELISA法检测肺组织中IL-17的水平。同时,采用HE染色法观察小鼠肺部气道的病理学变化。结果显示,在浓度为3.0 mg·m~(-3)的甲醛气体吸入染毒条件下,与对照组相比,1.5 h甲醛+OVA染毒组、2 h甲醛+OVA染毒组ROS、MDA、IL-17含量上升,具有统计学意义(P0.01)。同时,随着暴露时间长度的增加,小鼠肺部气道出现明显病理学变化。综上所述,每天2 h甲醛+OVA染毒能对小鼠肺造成损伤并恶化OVA对小鼠肺的损伤,产生炎症反应,并通过氧化应激反应介导。     

Inhibitory effect of antioxidants on the benz[a]anthracene-induced oxidative DNA damage in lymphocyte

Benz[a]anthracene is a ubiquitous environmental contaminant formed during the incomplete combustion of organic material. Some of the metabolites of benz[a]anthracene are known to be toxic and carcinogenic. In this investigation, benz[a]anthracene-induced oxidative damage to lymphocyte DNA was evaluated with the Comet assay (single cell gel electrophoresis). The level of oxidative DNA damage caused by benz[a]anthracene increased in a dose-dependent manner (24, 49) and oxidative DNA damage was significantly inhibited by 5 and 10 microg ml(-1) ascorbate, 5 microg ml(-1) polyphenols, as well as 5 and 10 microg ml(-1) curcumin. Moreover, traditional Korean medicinal herbs such as Acanthopanax and ginseng significantly reduced DNA damage. The results demonstrate that antioxidant supplementation to lymphocytes inhibits oxidative DNA damage in vitro, supporting an inhibitory effect against oxidative DNA damage, probably due to reduction of reactive oxygen species production induced by benz[a]anthracene.     

Dichloroacetate- and trichloroacetate-induced modulation of superoxide dismutase,catalase, and glutathione peroxidase activities and glutathione level in the livers of mice after subacute and subchronic exposures

Dichloroacetate (DCA) and trichloroacetate (TCA) were previously found to induce various levels of oxidative stress in the hepatic tissues of mice after subacute and subchronic exposures. The cells are known to have several protective mechanisms against production of oxidative stress by different xenobiotics. To assess the roles of the antioxidant enzymes and glutathione (GSH) in DCA- and TCA-induced oxidative stress, groups of B6C3F1 mice were administered either DCA or TCA at doses of 7.7, 77, 154, and 410 mg kg^?1 day^?1, by gavage for 4 weeks (4-W) and 13 weeks (13-W), and superoxide dismutase (SOD), catalase (CAT), and glutathione peroxidase (GSH-Px) activities, as well as GSH were determined in the hepatic tissues. DCA at doses ranging between 7.7–410, and 7.7–77 mg kg^?1 day^?1, given for 4-W and 13-W, respectively, resulted in either suppression or no change in SOD, CAT, and GSH-Px activities, but doses of 154–410 mg DCA kg^?1 day^?1 administered for 13-W were found to result in a significant induction of the three enzyme activities. TCA administration on the other hand, resulted in increases in the SOD and CAT activities, but caused suppression of GSH-Px activity in both the periods. Except for the DCA doses of 77–154 mg kg^?1 day^?1 administered for 13-W that resulted in a significant reduction in the GSH levels, all other DCA as well as TCA treatments produced no changes in GSH. Since these enzymes are involved in the detoxification of the reactive oxygen species (ROS), superoxide anion (SA), and H₂O₂, it is concluded that SA is the main contributor to DCA-induced oxidative stress, while both ROS contribute to that of TCA. The increase in the enzyme activities associated with 154–410 mg DCA kg^1? day^?1 in the 13-W period suggest their role as protective mechanisms contributing to the survival of cells modified in response to those treatments.     

苯酚的超临界水氧化试验

以自建的一套连续式超临界水氧化装置的温度，压力，溶氧量和流量等参数的可控性进行了实验，并在此基础上进行了苯酚的超临界水氧化研究。结果表明：所建立的装置能比较精确控制各种条件参数，是可靠的超临界水氧化试验研究装置。在氧气过量的条件下，停留时间是影响苯酚在超临界水中氧化分解的主要因素，反应的温度和压力升高导致苯致苯酚去除率的增大，只要有足够的氧气，苯酚起始浓度的增加对苯酚的转化率影响不明显，在实验条件下，溶液中苯酚的去除动力学对苯酚是一级，氧气是零级。