Fe、La掺杂和氧缺陷对CeO_(2)表面吸附As_(2)O_(3)的密度泛函理论研究

采用密度泛函理论研究了As_(2)O_(3)(g)在Fe、La掺杂CeO_(2)(110)表面及氧缺陷LaCeO(110)表面的吸附行为,探索了LaCeO表面砷吸附能力显著高于FeCeO表面的主要原因。结果表明,As_(2)O_(3)(g)的吸附效果与吸附位点数量、吸附能、键长和电荷转移密切相关。纯CeO_(2)表面的吸附主要为化学吸附,吸附能绝对值大于−4.22 eV,电荷转移量为(−0.19)−(−0.31)e,As_(2)O_(3)得到电荷带负电,起表面受主作用,因此吸附量较小。FeCeO(110)表面新增Fe顶位和Bridge-2桥位两个吸附位,其中,Fe顶位为化学吸附,Fe掺杂改变了FeCeO表面电子分布和晶格结构,但并未改变As_(2)O_(3)与FeCeO之间的电荷转移方向,因此,As_(2)O_(3)仍呈负离子形式吸附。LaCeO(110)表面新增了三个吸附位:La顶位、Bridge-3桥位和Hollow-2空位,La掺杂改变了As_(2)O_(3)与LaCeO之间的电荷转移方向,使得As_(2)O_(3)失电子呈正离子吸附,起表面施主作用,因此,吸附能力增强。无O_(2)环境下,单一O缺陷LaCeO(110)表面吸附能力低于完整LaCeO表面;有O_(2)环境下,O缺陷有利于As_(2)O_(3)的吸附。

As_(2)O_(3)与Cu-ZSM-5催化剂的相互作用机理

基于密度泛函理论计算了NO和As_(2)O_(3)在Cu-ZSM-5表面的吸附性能.通过确立As_(2)O_(3)在Cu-ZSM-5表面的最佳吸附位点,对As3+在其活性位点吸附的反应路径进行研究,计算As在催化剂上的吸附反应活化能垒和决速步骤,揭示As_(2)O_(3)与活性位点Cu-O-Cu的成键机制和相互作用机理.结果表明,NO和As_(2)O_(3)都以非氧端吸附在Cu-ZSM-5活性位点Cu-O-Cu的晶格氧位,吸附能分别为-218.515kJ/mol和-206.422kJ/mol,吸附过程中有电荷转移且发生了强烈的相互作用.As_(2)O_(3)在Cu-ZSM-5活性位点Cu-O-Cu的晶格氧上的氧化过程分两步进行,As^(3+)作为Lewis碱与Lewis酸中心的Cu-O-Cu发生非均相氧化反应,第一阶段的氧化产物As_(2)O_(4)在相邻的活性位点上发生二次氧化反应,生成的As_(2)O_(5)成为As^(3+)吸附后的主要存在形式.其中,生成As_(2)O_(4)的反应阶段需要跨越242.75kJ/mol的能垒,成为整个氧化进程的决速步骤.

南天竹根对抗肿瘤药As_(2)O_(3)减毒作用物质基础研究

目的研究南天竹根不同萃取部位对As_(2)O_(3)所致肝、肾毒性的保护作用,采用UPLC-Q-TOF-MS/MS技术探寻其减毒部位的主要化学成分。方法在As_(2)O_(3)致大鼠急性肝、肾损伤模型上,南天竹根70%乙醇提取物及其不同极性溶剂的萃取物灌胃后,记录各组大鼠体征变化,测定各组大鼠组织中肾脏系数、超氧化物歧化酶(Superoxide Dismutase,SOD)、过氧化氢酶(Catalase from micrococcus lysodeikticus,CAT)、丙二醛(Malondialdehyde,MDA),谷草转氨酶(Aspartate aminotransferase,AST)、谷丙转氨酶(Alanine aminotransferase,ALT)、内生肌酐清除率(Creatinine clearance rate,Ccr)、尿素氮(Blood urea nitrogen,BUN),HE染色检测大鼠肝、肾组织病理变化,以此筛选南天竹根的拮抗毒性部位,并采用UPLC-Q-TOF-MS/MS对拮抗毒性部位的化学成分进行分析鉴别。结果与模型组相比,各给药组大鼠的体征均呈现恢复趋势,肾脏系数、SOD、CAT、MDA、AST、ALT、Ccr、BUN等指标均得到了明显缓解,肝、肾病理损伤程度有所改善,其中以氯仿部位拮抗毒性效果最为明显。经LC-MS对氯仿部位分析鉴定发现,该部位共鉴定得到25个化合物,包括18个生物碱类成分。同时氯仿部位与主要单体成分——小檗碱对As_(2)O_(3)所致肝、肾毒性保护作用呈现剂量依赖性。结论表明南天竹根不同萃取部位对As_(2)O_(3)所致肝、肾毒性具有明显保护作用,其拮抗毒性成分可能为生物碱类成分。

γ-Fe_(2)O_(3)抗As_(2)O_(3)中毒能力的分子模拟

采用密度泛函理论研究了γ-Fe_(2)O_(3)表面As_(2)O_(3)的吸附以及掺杂改性提高抗As_(2)O_(3)中毒性能的作用机理.计算了As_(2)O_(3)在完整以及O缺陷γ-Fe_(2)O_(3)(001)表面的吸附性能,包括吸附位点、吸附结构、吸附能、PDOS等.同时建立了Mo、Ti、Mg掺杂的γ-Fe_(2)O_(3)模型,探讨了助剂掺杂对抗砷中毒能力的作用机制,并考虑了掺杂量的影响.结果表明:As_(2)O_(3)倾向于以O端化学吸附在γ-Fe_(2)O_(3)(001)表面Feoct位,吸附过程发生强烈的相互作用和电荷转移.当表面存在O缺陷时,As_(2)O_(3)的吸附能得到提高.Mo、Ti、Mg倾向于掺杂在Feoct位,增强了对As_(2)O_(3)的吸附能力,并且增大Mo的掺杂量可以强化As_(2)O_(3)的吸附.As_(2)O_(3)倾向于与活性较强的Mo、Ti、Mg发生反应,从而保护活性Fe位不受砷中毒,Ti和Mg的掺杂还抑制了相邻Fe位对As_(2)O_(3)的吸附.Mo、Ti、Mg的掺杂还促进了催化剂表面对NH_(3)的吸附,增强了表面酸性强度,有利于SCR反应.Mo、Ti、Mg原子的掺杂有利于提高γ-Fe_(2)O_(3)催化剂的抗砷中毒性能.

O_(2)、SO_(2)对As_(2)O_(3)在W-Cu/γ-Al_(2)O_(3)催化剂表面吸附特性的影响:实验及理论模拟

采用实验及量子化学方法探究了O_(2)和SO_(2)对As_(2)O_(3)在W-Cu/γ-Al_(2)O_(3)催化剂表面吸附特性的影响。实验结果表明,O_(2)促进了As_(2)O_(3)在催化剂表面的吸附,随着SO_(2)体积分数的增加,As_(2)O_(3)的吸附量表现出先升高后降低的趋势。为进一步探究烟气组分对气相砷吸附的影响机理,采用密度泛函理论(DFT)方法,模拟了预吸附不同气体后催化剂表面As_(2)O_(3)的吸附。结果表明,O_(2)对气相砷的促进影响主要归因于吸附氧的形成。预吸附的O原子明显增强了临近原子的吸附活性,而预吸附的O_(2)分子则主要通过提供吸附活性位点促进As_(2)O_(3)的吸附。SO_(2)在W-Cu/γ-Al_(2)O_(3)表面形成了SO_(4)^(2-)和HSO_(4)-,改变了基底表面的势场,从而促进了As_(2)O_(3)的吸附。随体积分数的进一步增加,SO_(2)与气相As_(2)O_(3)的竞争吸附作用增强,As_(2)O_(3)吸附量减少。

As_(2)O_(3)-PLA-NPs、As_(2)O_(3)-mPEG-PLA-NPs对肿瘤细胞MCF-7/ADR增殖和凋亡的影响

目的:制备三氧化二砷纳米粒并进行细胞学实验,分析体外药效及其对耐药细胞的逆转倍数。方法:运用CCK-8法考察纳米粒的细胞毒性以及纳米粒对乳腺癌细胞MCF-7/ADR多药耐药的逆转;采用Annexin V-FITC/PI双染法,用流式细胞仪检测三氧化二砷纳米粒诱导细胞凋亡的作用;采用PI单染流式细胞术检测As_(2)O_(3)-NPs对MCF-7/ADR周期的阻滞。结果:细胞学实验结果表明,各组药物均能够抑制耐药细胞的正常生长,凋亡率呈浓度依赖性,纳米粒组的凋亡率高于游离药物组;游离药物组和纳米粒组均阻滞细胞生长于G2/M期,As_(2)O_(3)-mPEG-PLA-NPs阻滞效果最好。As_(2)O_(3)、As_(2)O_(3)-PLA-NPs、As_(2)O_(3)-mPEG-PLA-NPs作为逆转剂时,ADM对MCF-7/ADR的逆转倍数分别为1.32、1.8和2.11。结论:As_(2)O_(3)-PLA-NPs、As_(2)O_(3)-mPEG-PLA-NPs均对乳腺癌耐药细胞MCF-7/ADR有促凋亡作用,对G2/M期细胞生长阻滞明显,对MCF-7/ADR的逆转作用强于As_(2)O_(3)。

Inhibitory effect of humanized anti-VEGFR-2 ScFv-As_2O_3-stealth nanoparticles conjugate on growth of human hepatocellular carcinoma:in vitro and in vivo studies

Objective:To investigate the inhibitory effect of humanized anti-VEGFR-2 ScFv-As2O3-stealth nanoparticles conjugate on growth of human hepatocellular carcinoma both in vitro and in vivo,which may be a potential agents with sensitivity and targeting ability for human hepatocellular cancer.Methods:Humanized anli-VECFR-2 ScFv-As2O3-stealth nanoparticles conjugate was previously constructed using ribosome display technology and antibody conjugate technology.In this combined in vitro and in vivo study,the inhibitory effects of anti-VEGFR-2 ScFv-As2O3-stealth nanoparticles conjugate on tumor growth,invasion,and metastasis was observed with human liver carcinoma cell line Bel7402 and normal cell L02 by MTT assay,Tanswell assay,Hochest33258 staining,and DNA ladder analysis.The anticancer activity and distribution of anti-VEGFR-2 ScFv-As2O3-stealth nanoparticles was then verified in a mouse model of Bel7402xenografts.Results:Anti-VEGFR-2 ScFv-As2O3-stealth nanoparticles significantly inhibited the proliferation of Bel7402 in the 3-(4,5-dimethylthiazol-2-yh-2,5-diphenyltetrazolium bromide assay while had almost no effects on L02 cells.And the apoptosis inducing effects were proved by Hochest33258 staining and DNA ladder analysis.Transwell assay found that the drug also inhibited the metastasis ability of tumor cells.Furthermore,anti-VEGFR-2 ScFv-As^-stealth nanoparticles significantly delayed the growth of Bel7402 xenografts after administration（92.9%）,followed by As2O3-stealth nanoparticles,anti-VEGFR-2 ScFv,and As203（61.4%,58.8%,20.5%,P【0.05）.The concentration of As2O3 in anti-VEGFR-2 ScFv-As2O3-steallh nanoparticles group was more selectively.Conclusions:Anti-VEGFR-2 ScFv-As2O3-stealth nanoparticles is a potent and selective anti-hepatocellular carcinoma agent which could inhibit the growth of liver cancer as a targeting agent both in vitro and in vivo and also significantly inhibit angiogenesis.

Influence of As_2O_3 combined with ginsenosides Rg3 on inhibition of lung cancer NCI-H1299 cells and on subsistence of nude mice bearing hepatoma

Objective:To study the effect of arsenic trioxide（As2O3）combined with ginsenosides Rg3 on inhibiting the NCI-H1299 lung cancer cells and subsistence in nude mice bearing hepatoma.Methods:MTT method was used to measure the inhibition effect of（As2O3）combined Rg3 on NC1-H1299 cells,and the proliferation inhibiting effect was observed via establishing the transplanted tumor model in vitro.A total of 40 tumor-bearing nude mice were randomly divided into normal saline group,（As2O3）,Rg3 and As2O3+Rg3 group.Transplantation tumor model of lung cancer in nude mice was constructed,followed by injection of certain concentrations of normal saline,As2O3,ginseng saponin Rg3 and As2O3+Rg3 every day.The survival duration and the tumors size of the mice were recorded and the Kaplan-Meier curve was made;microscopic observation of apoptosis of tumor cells in vivo was done using TUNEL staining.Results:After 72 h of injection.inhibition rate of tumor cell in normal saline group,As2O3 group.Rg3 group and As2O3+Rg3 group was（5.66±0.31）%,（65.58±4.75）%,（44.69±3.32）%and（82.67±5.43）%,respectively.Inhibition rate of tumor cell in As2O3 group.Rg3 groap and As2O3+Rg3 group was significantly higher than that of normal saline group（P【0.01）;inhibition rate of tumor cells of As2O3+Rg3 group was significantly higher than that of the two groups given As2O3 or Rg3 alone（P【0.01）.The tumor volume of As2O3 group,Rg3 group and As2O3+Rg3 group shrank to（65.38±3.25）%,（77.68±3.43）%and（42.65±3.55）%of the original,tumor volume of saline group was 1.21 times of the original size（P【0.01）;Median survival of saline group,Rg3 group,As2O3 group were significantly shorter than that of As2O3+Rg3 group（P【0.01）;co-ordinated intervention ability of As2O3+Rg3 on NCI-H1299 cell was significantly higher than that of As2O3 or Rg3,separately.Conclusions:As2O3 combined with Rg3 can significantly inhibit prolifaration of NCI-H1299 cells in lung cancer,prolong survival fo tumor-bearing nude mice,and promote tumor cell apoptosis,and have significant effect on lung cancer treatment.

从高砷铅阳极泥中回收As_(2)O_(3)试验研究

研究了从高砷铅阳极泥中回收砷,提出了“碱性加压浸出—浸出液浓缩结晶砷酸钠—砷酸钠溶解还原制备三氧化二砷”工艺。结果表明:适宜条件下,铅阳极泥中砷脱除率在87%以上;整个流程砷直收率在65%以上,所得As_(2)O_(3)产品纯度在99%以上。

二维As_(2)O_(3)光催化性质理论研究

基于密度泛函理论的超软赝势第一性原理计算方法,该文提出了一种新型P-3m1相二维As_(2)O_(3),并研究其结构稳定性,电子结构和光催化性质.计算结果显示,二维As_(2)O_(3)具备较好的稳定性,并具有1.04 eV的间接能隙.基于形变势理论进一步计算了As_(2)O_(3)的载流子迁移率,发现其电子和空穴的迁移率表现出明显的各向异性,沿armchair和zigzag方向的电子/空穴迁移率分别为1259.91/115.41 cm^(2)·V^(-1)·s^(-1)和1254.21/36.12 cm^(2)·V^(-1)·s^(-1),这说明As_(2)O_(3)具备很低的电子-空穴复合率,拥有较高的光催化活性.对比标准氢电极的氧化还原势发现,二维As_(2)O_(3)具备2.57 eV的氧化势能,能够光催化水裂解出O_(3),O_(2)和H_(2)O_(2)等.此外,二维As_(2)O_(3)对可见光和紫外光表现出强烈的吸收效果,吸收系数高达10^(5) cm^(-1).这表明二维As_(2)O_(3)在纳米电子器件和光催化领域有着潜在的应用前景.

钒-砷氧簇合物[Zn_(2)(dien)_(3)]_(1/2){[Zn_(2)(dien)_(3)]As_(6)V_(15)O_(42)}·2H_(2)O的合成与晶体结构表征

本文以氯化锌、五氧化二钒以及三氧化二砷为原料,合成了[Zn_(2)(dien)_(3)]_(1/2){[Zn_(2)(dien)_(3)]As_(6)V_(15)O_(42)}·2H_(2)O,讨论了其晶体结构并进行了结构表征。

硫酸负载对Pt/SO_(4)^(2-)-(ZrO_(2)-Al_(2)O_(3))催化剂性能的影响

采用共沉淀-浸渍法制备了系列硫酸负载催化剂Pt/SO_(4)^(2-)-(ZrO_(2)-Al_(2)O_(3)),利用X射线衍射仪、物理吸附仪、红外光谱仪等对其进行了表征,并在固定床微型反应装置上对其催化异丁烷正构化反应性能进行了评价。结果表明:硫酸单层分散于载体表面,硫酸负载不利于四方晶相ZrO_(2)长大;随着硫酸负载量的增加,催化剂介孔结构的有序性增强且孔径减小,孔径最小降为3.41 nm,孔容可提高至0.091 cm^(3)/g,比表面积增至100 m^(2)/g以上;在反应温度为250℃的条件下,硫酸负载量为15%时,异丁烷转化率高达41.74%;硫酸负载量为2%时,正丁烷选择性最高为93.91%。

As_(2)O_(3)饮水慢性中毒对大鼠肝脏TRβ1介导的甲状腺激素信号通路的影响

As_(2)O_(3)能干扰大鼠血清甲状腺激素(TH)水平,引发慢性肝损伤,然而其机制仍不清楚。为了探明TH信号通路在As2O3引发慢性肝损伤中的作用,采用qRT-PCR、Western blot技术检测大鼠肝脏TH信号通路的关键调控因子TRβ1、核内途径TRβ1的下游因子(Cyclin D1)基因和蛋白表达变化,核外途经关键因子(Bax、Bcl-2)蛋白的变化。结果显示:与对照组相比,As_(2)O_(3)作用110d,雌鼠肝脏TRβ1蛋白表达均显著降低(P<0.01),0.1、0.2mg/L组Cyclin D1表达显著升高(P<0.01);雄鼠0.4mg/L组TRβ1蛋白表达显著降低(P<0.01),各组Cyclin D1的表达均显著升高(P<0.01),mRNA表达结果与蛋白基本一致。与对照组相比,As_(2)O_(3)作用194d,各组TRβ1蛋白表达显著降低(P<0.01),Cyclin D1的表达均显著升高(P<0.01),mRNA表达结果与蛋白基本一致。与对照组相比,As_(2)O_(3)干扰了大鼠Bcl-2和Bax蛋白表达,并随着作用时间的增长,诱导Bcl-2/Bax蛋白比值升高。其中,各组雌鼠和0.4mg/L组雄鼠Bcl-2/Bax比值显著升高(P<0.01),0.1mg/L组雄鼠明显升高(P<0.05)。表明大鼠长期慢性饮水摄入As_(2)O_(3)会引起其肝脏TRβ1的基因和蛋白水平异常下降,Cyclin D1的水平异常升高,诱导Bcl-2/Bax蛋白比值升高。

全反式维甲酸联合As_(2)O_(3)对初发急性早幼粒细胞白血病患者体内相关基因表达的影响

目的 研究全反式维甲酸联合三氧化二砷(As_(2)O_(3))对初发急性早幼粒细胞白血病(APL)患者体内相关基因表达的影响。方法 选择2014年3月-2017年6月首次在喀什地区第一人民医院诊断为APL的50例患者,根据治疗方案不同分为接受全反式维甲酸联合As_(2)O_(3)治疗的观察组24例,全反式维甲酸联合化疗的对照组26例。治疗前及治疗后14、28 d,测定骨髓中增殖、凋亡、侵袭相关基因的表达水平。结果 与治疗前比较,两组治疗后2周、4周时骨髓中增殖相关基因染色体10上缺失的磷酸酶与张力蛋白同源物基因(PTEN)、凋亡相关基因Bcl-2相关X蛋白(BAX)、高温需求蛋白A2(HtrA2)、含半胱氨酸的天冬氨酸蛋白水解酶-3(Caspase-3)、基质金属蛋白酶组织抑制因子(TIMP)1、TIMP2的mRNA表达水平升高,C-myc、细胞周期蛋白B1(CyclinB1)、周期蛋白依赖性激酶1(CDK1)、细胞FLICE样抑制蛋白(c FLIP)、生存素、侵袭相关基因基质金属蛋白酶(MMP)2、MMP9、CXC趋化因子受体(CXCR)4、CXCR7的mRNA表达水平降低,差异有统计学意义(P<0.05);观察组治疗后2周、4周时骨髓中PTEN、BAX、HtrA2、Caspase-3、TIMP1、TIMP2的mRNA表达水平均高于对照组,C-myc、CyclinB1、CDK1、cFLIP、生存素、MMP2、MMP9、CXCR4、CXCR7的mRNA表达水平均低于对照组,差异有统计学意义(P<0.05)。结论 全反式维甲酸联合As_(2)O_(3)治疗初发APL能够明显调控增殖、凋亡、侵袭相关基因的表达。

As_(2)O_(3)对大鼠BRL-3A和RH-35细胞TRβ1和Cyclin D1因子的影响

为了探明As_(2)O_(3)对大鼠肝脏细胞系BRL-3A和肝癌细胞系RH-35中TH信号通路的关键调控因子TRβ1和TRβ1的下游因子Cyclin D1的影响,采用qRT-PCR、Western blot技术检测2种细胞中TRβ1和Cyclin D1的基因和蛋白表达变化。结果显示:(1)与对照组相比,As_(2)O_(3)作用BRL-3A细胞12h,1.563μmol/L组TRβ1蛋白表达显著降低(P<0.01)、Cyclin D1表达显著升高(P<0.01);6.250μmol/L组TRβ1表达明显降低(P<0.05)、Cyclin D1表达显著降低(P<0.01)。As_(2)O_(3)作用24h,1.563μmol/L组TRβ1蛋白表达明显升高(P<0.05);6.250μmol/L组TRβ1显著升高(P<0.01),Cyclin D1的表达显著降低(P<0.01)。As_(2)O_(3)作用48h,6.250μmol/L组TRβ1蛋白表达显著升高(P<0.01),各组Cyclin D1表达均显著降低(P<0.01)。基因表达结果与蛋白表达结果基本一致。(2)与对照组相比,As_(2)O_(3)作用RH-35细胞12h,各组TRβ1蛋白表达量显著升高(P<0.01)。As_(2)O_(3)作用RH-3524h,1.563μmol/L组TRβ1蛋白表达量明显升高(P<0.05),其余组显著升高(P<0.01)。As_(2)O_(3)作用48h,3.125和6.250μmol/L组TRβ1蛋白表达显著升高(P<0.01),1.563μmol/L组明显降低(P<0.05)。As_(2)O_(3)作用RH-3512,24,48h,各组Cyclin D1蛋白表达量均显著降低(P<0.01)。基因结果与蛋白结果基本一致。表明As_(2)O_(3)随着作用时间的增加,引起大鼠肝脏细胞系BRL-3A和肝癌细胞系RH-35TRβ1的水平异常,进而干扰Cyclin D1的水平。

Arsenic trioxide inhibits the activity of SphK1 by decreasing the level of phosphatidylserine and phosphatidic acid in the human gastric cancer cell line MGC-803

Sphingosine kinase 1(SphK1)is an important synthetase during the synthesis of sphingosine-1-phosphate(S1P)from sphingosine(Sph).Previous studies demonstrated that arsenic trioxide(As_(2)O_(3))could reduce the level of S1P in human gastric cancer cell line MGC-803,indicating that As_(2)O_(3) may inhibit the activity of SphK1.In this study,the effect of As_(2)O_(3) on the SphK1 activation pathway was investigated.Western blot and quantitative real-time PCR analysis were used to evaluate the changes in protein and mRNA levels.The multi-dimensional mass spectrometry-based shotgun lipidomics method(MDMS-SL)was used for the quantitative detection of phosphatidylserine(PS)and phosphatidic acid(PA).The results revealed that As_(2)O_(3) did not affect the protein and mRNA expression of SphK1 in the MGC-803 cells.However,As_(2)O_(3) increased the levels of p-ERK1/2 and CIB1 in the SphK1 activation pathway and decreased the levels of PS and PA in the MGC-803 cells.The outcomes suggested that As_(2)O_(3) may enhance the activity of SphK1 by increasing the levels of p-ERK1/2 and CIB1 and decrease the activity of SphK1 by decreasing the levels of PS and PA.It was suggested that the inhibition effect is stronger and resulting in an overall decrease in the activity of SphK1.

三氧化二砷联合^(125)I粒子植入抑制肺癌移植瘤小鼠肿瘤生长

观察不同剂量As_(2)O_(3)联合^(125)I粒子植入对肺癌移植瘤小鼠的抑瘤作用和安全性。构建肺癌异种移植瘤小鼠模型,当肿瘤体积达到约300 mm 3时,将小鼠随机分为6组,连续治疗15 d。测量小鼠肿瘤瘤径、体重、饮食,检测小鼠血清ALT、AST、LDH、CK、BUN、Cr浓度及脏器指数,HE染色评估主要脏器组织病理学变化。结果显示:与模型组相比,单用As_(2)O_(3)以及As_(2)O_(3)联合^(125)I粒子植入使小鼠饮食量和体重减少;单用As_(2)O_(3)(2.5 mg/kg、5 mg/kg)、^(125)I粒子(0.7 mci)治疗组以及联合治疗组均能明显抑制小鼠肿瘤生长(P<0.05);联合治疗组抑制作用优于单用As_(2)O_(3)和^(125)I粒子植入组(P<0.001);联合治疗组对小鼠血清生化功能及脏器指数无明显影响(P>0.05),组织病理学观察未见明显异常。综上,As_(2)O_(3)联合^(125)I粒子植入能够抑制肺癌移植瘤小鼠肿瘤生长,且优于单用As_(2)O_(3)和^(125)I粒子植入,方法安全可行。

IGF2信号通路在As_(2)O_(3)致GC-2细胞凋亡中的作用

砷是一种天然类金属化学元素,广泛存在于自然界中,是世界卫生组织公布的引起重大公共关注的10种危害环境与健康的化学品之一^([1])。砷也是一种雄性生殖毒物,可以下调精子质量^([2])。流行病学报告显示,饮用水中砷含量超标导致男性血液和精液中砷含量明显升高,并造成男性精子数量和精子存活率的下降[3-4]。动物实验也发现,慢性砷暴露降低小鼠精子质量[5-6]。IGF2(胰岛素样生长因子2)信号通路是与男性生殖关系密切的信号通路.

雄黄毒性研究进展

雄黄具有解毒杀虫、燥湿祛痰、截疟的功效,适用于多种病症,临床主要用于治疗痈肿疔疮、蛇虫咬伤、虫积腹痛、惊痫及疟疾等。现代研究表明雄黄对血液系统疾病、恶性淋巴系统疾病以及实体瘤等具有良好的治疗作用,尤其对白血病的疗效颇为显著。雄黄作为一种有毒的含砷矿物药,若使用不当,其毒性也不容忽视。雄黄发挥治疗作用或毒性作用的成分为可溶性砷,包括无机砷和有机砷。雄黄具有中枢神经系统毒性、肝脏毒性及遗传毒性作用,合理配伍可以降低雄黄的毒性。炮制对雄黄的毒性有影响,水飞法炮制的雄黄毒性更低,目前也有研究者采用微生物转化、纳米技术等新技术对雄黄毒性进行研究。本文通过对雄黄毒性进行综述,以期为雄黄的安全合理用药提供理论依据。

On the monolayer dispersion behavior of Co_(3)O_(4)on HZSM-5 support:designing applicable catalysts for selective catalytic reduction of nitrogen oxides by ammonia

Based on monolayer dispersion theory,Co_(3)O_(4)/ZSM-5 catalysts with different loadings have been prepared for selective catalytic reduction of nitrogen oxides by ammonia.Co_(3)O_(4)can spontaneously disperse on HZSM-5 support with a monolayer dispersion threshold of 0.061 mmol 100 m^(-2),equaling to a weight percentage around 4.5%.It has been revealed that the quantities of surface active oxygen(O_(2)^(-))and acid sites are crucial for the reaction,which can adsorb and activate NO_(x)and NH_(3)reactants effectively.Below the monolayer dispersion threshold,Co_(3)O_(4)is finely dispersed as sub-monolayers or monolayers and in an amorphous state,which is favorable to generate the two kinds of active sites,hence promoting the performance of ammonia selective catalytic reduction of nitrogen oxide.However,the formation of crystalline Co_(3)O_(4)above the capacity is harmful to the reaction performance.4%Co_(3)O_(4)/ZSM-5,the catalyst close to the monolayer dispersion capacity,possesses the most abundant active O_(2)^(-)species and acidic sites,thereby demonstrating the best reaction performance in all the samples.It is proposed the optimal Co_(3)O_(4)/ZSM-5 catalyst can be prepared by loading the capacity amount of Co_(3)O_(4)onto HZSM-5 support.