附子中双酯型乌头碱类成分水解减毒机理的密度泛函理论研究

采用密度泛函理论B3LYP/6-31G*方法,对附子中的9种乌头碱类成分进行了量子化学理论研究,讨论了该类生物碱的结构和毒性的关系.结果表明,由于水解过程中C(8)和C(14)上基团的变化影响了分子的构型、电荷分布、前线分子轨道等性质,使分子与受体之间的作用减弱,毒性降低,生物碱分子的正电区域是发生作用的活性中心.     

氯酚化合物对发光细菌毒性的构效关系研究

本文对20种氯酚化合物进行DFT-B3LYP/6-311G**水平全优化计算,据所得量子化学参数构建其对发光细菌毒性的定量构效关系(QSAR)模型。经逐步多元回归分析后,所建立的QSAR模型的相关系数R及去一法(LOO)交互检验复相关系数R2cv分别为0.962和0.876;用预测集样本进行了外部预测,所得外部预测集交互检验Q2ext为0.961,表明所建立的QSAR模型具有较好的稳定性和较强的预测能力。结果表明:分子的体积愈大,化合物毒性愈强;最负非氢原子净电荷愈负,毒性愈强。对模型应用域(AD)进行了表征,所建立的模型可以应用于应用域内氯酚化合物对发光细菌毒性的预测,具有潜在应用价值。     

一类新型荧光化学敏感器形成激基缔合物的温度效应

对一类具有分子识别功能的荧光分子敏感器化合物，在水溶液中形成的分子内激基缔合物的温度效应进行了研究。进而提出该类化合物在水溶液中进行了内单体和分子内激基缔合物转化的机制。通过分析所得的热力学数据，同文献值相比较，推导出该类化合物在水溶液中可能存在的几何构型，为该类化合物在作为探针应用时提供理论依据。     

二氧化钛分子电致发光激发特性研究

采用密度泛函B3P86方法优化得到了沿分子平面不同外电场作用下TiO₂分子的基态稳定构型, 在优化构型下利用杂化CIS (CI-Singles)-B3P86方法在6-311＋G*基组水平上, 研究了不同外电场下TiO₂分子前六个激发态的激发能和跃迁波长等激发特性. 研究结果表明, TiO₂分子多个激发态满足偶极跃迁定则, 跃迁光谱对应多个峰值, 在分子水平上, 可以增大利用太阳光的比例. 在外电场作用下, 能隙随电场的增大而减小, 电子易从最高占据轨道跃迁到最低空轨道形成空穴, 各个激发态跃迁波长均有随电场增大发生红移的趋势, 最长589 nm, 因而利用外电场可以控制材料的发光光谱范围在可见光区域扩展.     

外电场作用下甲基乙烯基硅酮分子结构和电子光谱

采用密度泛函B3P86方法在6-311++G(d, p)基组水平上优化得到了沿分子轴方向不同外电场(0-0.04 a.u.)作用下, 甲基乙烯基硅酮分子的基态电子状态、几何结构、电偶极矩和分子总能量. 在优化构型下利用杂化CIS-DFT方法(CIS-B3P86)研究了同样外电场条件下对甲基乙烯基硅酮的激发能和振子强度的影响. 计算结果表明, 分子几何构型与电场大小呈现强烈的依赖关系, 分子偶极矩μ随电场的增加先减小后急剧增大. 电场为零时, 分子总能量为-483.5532137 a.u., 随着电场增加, 能量升高, 在F=0.02 a.u.时达到最大值-483.5393952 a.u., 此后, 继续增大电场系统总能量则开始降低. 激发能随电场增加急剧减小, 表明在电场作用下, 分子易于激发和离解.     

系列二羰基化合物的HeI紫外光电子能谱(UPS)及量子化学研究

报道了醌及苯并酸酐等系列二羰基化合物的气相HeI紫外光电子能谱。对各体系利用Gaussian94程序RHF/3-21G进行了构型优化,对得到的优势构型采用STO-6G基组进行了轨道计算。并结合计算结果对各分子体系的UPS谱进行了分析指认。计算结果分析显示:标题化合物的第一个电离峰均是由苯环部分的共轭π键电子电离及羰基的孤对电子电离引起的,且化合物的IP~1值随羰基在HOMO轨道中权重的增大而增大。各化合物的第二、三谱带都与羰基不同类型的孤对电子峰相关联。说明羰基为此类化合物的特征基团。且分子的对称性越高,羰基的孤对电子峰n^-和n^+的平均值越大,分裂值也越大。     

类杯芳烃孔穴桥联双芘分子开关化合物

利用构型可变的分子开关类杯芳烃孔穴化合物(Cavitand)作为母体,合成了2种具有不同臂长的双芘Cavitand化合物.在室温及中性状态下,2种双芘Cavitand化合物均可检验出分子内激基复合物荧光,其中短臂双芘Cavitand化合物的荧光明显强于长臂Cavitand化合物.经三氟乙酸酸化后,2种双芘化合物的分子内激基复合物荧光消失;而继续使用碱中和至中性,则荧光恢复.这个荧光出现-消失-出现的过程验证了Cavitand母体化合物分子构型闭合-打开-闭合可有效调控分子激基复合物荧光开关过程.此外,通过高斯计算模拟了2种化合物的理论分子构型,发现长臂双芘化合物在Cavitand母体构型处于闭合状态时2个芘基团重叠部分较少是其分子内激基复合物荧光较弱的关键原因.     

电子辐照及再结晶P(VDF-TrFE)共聚薄膜红外光谱研究

利用傅立叶变换红外光谱(FT-IR)研究聚偏氟乙烯与聚三氟乙烯共聚薄膜[P(VDF0.80-TrFE0.20)]的电子辐照和再结晶处理过程中分子链构型变化和化学变化, 为深入探讨辐照的改性机理提供依据. 研究发现, 辐照后薄膜分子链全反构型百分含量随吸收剂量增大而迅速减少, TG构型和T3G构型百分含量显著增多. 而当吸收达一定剂量时, 三种构型相对含量基本不再变化, 表明高剂量辐照时样品极性回升不依赖分子链构型中全反型的含量的增多, 而是和高交联度的边界效应有关. 再结晶过程中分子链构型变化恰好和辐照效应产生的变化相反, 并且形成了更加稳定的C=C共轭结构.     

苯及其含氮等电子体化合物的结构和性质的理论研究

采用密度泛函理论的B3LYP方法在aug-cc-pvDZ基组上研究了13种苯及其含氮等电子体化合物的分子结构、 能量和异构体相对稳定性, 重点考察了含氮量对化合物含能性质的影响. 结果表明: 随着氮原子数增加分子的总能量降低, 且存在很好的线性相关性. 采用G3方法对分子的生成热进行了计算, 结果显示随着分子中氮原子个数增加, 各含氮等电子体化合物的生成热将增大, 其中六嗪、五嗪的生成热较大, 它们成为含能材料的潜力较大. 对各异构体分析显示, 氮原子位置与总能量和生成热的关系均为: (邻)间位＜(邻)对位＜邻位. 此外, 通过NBO方法分析了分子的超共轭作用和立体排斥能对异构体稳定性的影响, 结果表明超共轭作用是影响各异构体构型相对稳定性的主要因素.     

激子手性方法用于多氧取代环己烯类化合物的研究

多氧取代环己烯是一类比较独特的天然产物,分子中多具有四个手性中心,立体化学多变,尽管用化学衍生物方法确定了部分化合物的绝对构型,但对已报道的化合物中仍有大部分未能确定其构型。在阐明分子相对构型的基础上,应用激子手性方法确定此类化合物的绝对构型,并利用Alchemy程序进行了分子动力学计算,对此类化合物的圆二色性规律进行了总结。     

pH-Sensitive surfactants from lysine: assessment of their cytotoxicity and environmental behavior

The toxicity and environmental behavior of new pH-sensitive surfactants from lysine are presented. Three different chemical structures are studied: surfactants with one amino acid and one alkyl chain, surfactants with two amino acids on the polar head and one alkyl chain, and gemini surfactants. The pH sensitivity of these compounds can be tuned by modifying their chemical structures. Cytotoxicity has been evaluated using erythrocytes and fibroblast cells. The toxic effects against these cells depend on the hydrophobicity of the molecules as well as their cationic charge density. The effect of hydrophobicity and cationic charge density on toxicity is different for each type of cells. For erythrocytes, the toxicity increases as hydrophobicity and charge density increases. Nevertheless, for fibroblasts cationic charge density affects cytotoxicity in the opposite way: the higher charge density, the lower the toxicity. The effect of the pH on hemolysis has been evaluated in detail. The aquatic toxicity was established using Daphnia magna . All surfactants yielded EC(50) values considerably higher than that reported for cationic surfactants based on quaternary ammonium groups. Finally, their biodegradability was evaluated using the CO(2) headspace test (ISO 14593). These lysine derivatives showed high levels of biodegradation under aerobic conditions and can be classified as "readily biodegradable compounds".     

Ultrahigh reactivity and grave nanotoxicity of copper nanoparticles

Recently, it was reported that the toxicity of copper particles increases with the decrease of the particle size on a mass basis. To understand this phenomenon, inductively coupled plasma mass spectrometry (ICP-MS) techniques and in vitro chemical studies were carried out to explore how they produce toxicity in vivo. The results suggest that when the sizes of particles become small and down to a nanoscale, copper becomes extremely reactive in a simulative intracorporeal environment. The nanosized copper particles consume the hydrogen ions in stomach more quickly than micron ones. These processes further convert the copper nanoparticles into cupric ions whose toxicity is very high in vivo.     

An investigation of chlorophenol proton affinities and their influence on the biological activity of microorganisms

The proton affinities of 15 chlorophenols are calculated by ab initio methods. Straight correlation between proton affinities and changes in the electronic structure is observed. The proton affinities decrease linearly with the electronic density gain on the chlorine atoms, as the liberation of the proton increases. To confirm the importance of the proton affinities on the toxicity of chlorophenols, calorimetric responses of these molecules and related ones where the acid proton is changed to a methyl group (anisol and its chlorinated derivatives) were used to verify their effects on Chromobacterium violaceum. The results confirmed that the chlorophenols are more toxic than the respective chloroanisols and suggest that high proton affinities are associated with low toxic activity. The toxicity of the chlorophenols can be associated with the respiratory mechanism in some microorganisms.     

Synthesis of Nonionic Oligomeric Manganese（ Ⅱ ） Complexes and Investigation of Their Toxicity and T1 -Relaxation Enhancement

Six nonionic oligomeric manganese （ Ⅱ ） complexes with oligomeric phosphate-polyglycol-EDTA ester ligands were synthesized and characterized. The longitudinal relaxivities of these complexes were measured. One of these complexes, which showed the highest relaxivity, was chosen to be used in the acute toxicity test and the T1-weighted imaging experiment. It has been found that compared to Gd-DTPA, this nonionic oligomeric Mn（ Ⅱ ） complex exhibits no acute toxicity, generates highly enhanced MRI signals and increases the intention time in the rat liver tissue.     

Toxicity analysis of second use lithium-ion battery separator and electrolyte

Pyrolysis gas chromatography-mass spectrometry (Py-GC-MS) test, smoke toxicity analysis and mouse biological toxicity test were carried out on the second use lithium-ion battery separator and electrolyte. It was found that the types of cracked products of separator and electrolyte under different state of health (SOH) were basically the same, mainly phosphoryl fluoride (POF₃) and long-chain F-containing alkanes, alcohols and esters. The content of POF₃ in the cracked product increases as the SOH increases. The toxic gas components released after the separator and the electrolyte are completely burned mainly include CO, CO₂, and HF. The HF content decreased as the battery SOH decreased, from 101.6 mg/g of the 100% SOH battery to 44.1 mg/g of the 65% SOH battery. In the biological toxicity test, all the mice were found to stop running, close eyes, shed tears, and have shortness of breath. After the test, only 65% SOH and 100% SOH mice recovered their body weight to the pre-experimental average state and gained weight.     

A Comparative Analysis of In Vitro Toxicity of Synthetic Zeolites on IMR-90 Human Lung Fibroblast Cells

Broad industrial application of zeolites increases the opportunity of inhalation. However, the potential impact of different types and compositions of zeolite on cytotoxicity is still unknown. Four types of synthetic zeolites have been prepared for assessing the effect on lung fibroblast: two zeolite L (LTL-R and LTL-D), ZSM-5 (MFI-S), and faujasite (FAU-S). The cytotoxicity of zeolites on human lung fibroblast (IMR-90) was assessed using WST1 cell proliferation assay, mitochondrial function, membrane leakage of lactate dehydrogenase, reduced glutathione levels, and mitochondrial membrane potential were assessed under control. Intracellular changes were examined using transmission electron microscopy (TEM). Toxicity-related gene expressions were evaluated by PCR array. The result showed significantly higher toxicity in IMR-90 cells with FAU-S than LTL-R, LTL-D and MFI-S exposure. TEM showed FAU-S, spheroidal zeolite with a low Si/Al ratio, was readily internalized forming numerous phagosomes in IMR-90 cells, while the largest and disc-shaped zeolites showed the lowest toxicity and were located in submembranous phagosomes in IMR-90 cells. Differential expression of TNF related genes was detected using PCR arrays and confirmed using qRT-PCR analysis of selected genes. Collectively, the exposure of different zeolites shows different toxicity on IMR-90 cells.     

UGT1A1*28基因多态性与伊立替康治疗晚期非小细胞肺癌的毒副反应及疗效的关系研究

目的探讨UGT1A1*28基因多态性与CPT-11治疗晚期NSCLC的毒副反应与疗效的关系。方法外周血检测2015年6月至2016年6月在九江市第一人民医院所收治的50例晚期NSCLC患者UGTIA1*28 TATA盒基因序列,并对所有50例患者接受CPT-11为基础化疗方案的患者出现的不良反应和近期疗效随访记录,比较不同基因型之间的差别。结果 50例晚期NSCLC患者中UGTIA1*28位点突变型可以增加发生3级以上腹泻(P=0.007)和3级以上血小板减少(41.7%VS 10.5%,P=0.027)的风险。结论在CPT-11化疗的患者中,UGTl Al*28基因型TA6/7,或TA7/7基因型可增加晚期NSCLC患者发生Ⅲ度以上腹泻及血小板减少的风险,然而不影响化疗的近期疗效。     

Radiolysis of paracetamol in dilute aqueous solution

Using radiolytic experiments hydroxyl radical (main reactant in advanced oxidation processes) was shown to effectively destroy paracetamol molecules. The basic reaction is attachment to the ring. The hydroxy-cyclohexadienyl radical produced in the further reactions may transform to hydroxylated paracetamol derivatives or to quinone type molecules and acetamide. The initial efficiency of aromatic ring destruction in the absence of dissolved O₂ is c.a. 10%. The efficiency is 2–3 times higher in the presence of O₂ due to its reaction with intermediate hydroxy-cyclohexadienyl radical and the subsequent ring destruction reactions through peroxi radical. Upon irradiation the toxicity of solutions at low doses increases with the dose and then at higher doses it decreases. This is due to formation of compounds with higher toxicity than paracetamol (e.g. acetamide, hidroquinone). These products, however, are highly sensitive to irradiation and degrade easily.     

Discriminating toxicant classes by mode of action: 3. Substructure indicators

Decision support for selecting suitable QSARs for predictive purposes is suggested by a stepwise procedure: The first tier pre-filters the compounds based on substructure indicators for baseline versus excess toxicity. This step, if sufficiently conservative, discriminates chemicals, whose toxicity can be reliably estimated from their log KOW from those, that require further classification by biological and chemical domain. A test set of 115 chemicals from 9 different MOA classes was used to compare the discriminatory power of several classification schemes based on substructure indicators. Performance, evaluated by contingency table statistics, is varied and no single scheme provides sufficient applicability and reliability for pre-filtering chemical inventories. Major improvements are feasible with combined use of three classification schemes: assignments of baseline toxicants are protective, recognition of excess toxicants is acceptable and applicability range increases favourably.     

Effect of Deacetylation on Statmhokinetic Activity of Colchicine Derivatives

Screening of colchicine derivatives that was carried out with the tumor culture CaPa in a cytotoxicity test showed that deacetylation decreases the cytotoxicity and increases the mitotic index. Lower toxicity of the deacetylated colchicine derivatives was also noted.