硫化物纳米级粒子化膜的形成与气相性质的影响

采用偏振光反光度、紫外及可见光谱、电子显微镜形貌观察、粒子大小测定及电子衍射等方法加以系统研究硫化锌纳米级粒子化膜的制备与气相性质的影响．     

Voltammetric studies of the effect of Cisplatin-liposome on Hela cells

In this paper, the voltammetric method was used for the first time to study the effect of Cisplatin-liposome on Hela cells. The results showed the voltammetric behavior of Hela cells was irreversible and the peak current had linear relationship with the cell number. With both Cisplatin-liposome concentration and treating time increasing, the peak current decreased. The peak current decreasing was in accordance with the nuclear damage and loss of mitochondrial membrane potential revealed by two-photon laser scanning microscopy and confocal laser scanning microscopy. This voltammetric method may provide a simple way to study the electron-transfer mechanism in drug-treating cells.     

A kinetic stability study of MN (MBe,Mg, Ca,Sr, and Ba)

This work describes a structure and kinetic stability study of some complexes with the general formula MN, where M are the alkaline earth metal atoms, Be, Mg, Ca, Sr, and Ba. A complex (A) with two points of attachment to the N₅ ring is the most energetically favored for all metals considered here. Except for Be, structure (B) containing a mono‐coordinated metal atom is a transition state corresponding to the metal atom transfer around the N₅ ring. Pyramidal structure (C) is kinetically unstable with the low isomerization barrier height, ranging from 0.9 to 6.7 kcal/mol. The dissociation barrier heights for the lowest energy isomers (A) are predicted to be 1.2–18.7 kcal/mol (Be to Ba), indicating that kinetic stability increases from lighter to heavier metal atoms. © 2004 Wiley Periodicals, Inc. Int J Quantum Chem, 2004     

激光拉曼光谱在高分子中的应用

论述了激光拉曼光谱对高分子结构、结晶形态和表征,反应动力学过程和取向的研究,还介绍了纵向声学模、共振、高温高压、光波导和付里叶拉曼光谱在高分子研究中的最新进展。     

醛的自氧化振荡反应

1983年 Jensen 与 Roelofs 等报道了苯甲醛自氧化反应中出现的化学振荡现象。我们还观察到苯甲醛、取代苯甲醛和许多脂肪醛的自氧化振荡反应,实验方法与文献[3]相似。反应在具有电磁搅拌的恒温反应器中进行,以醋酸水溶液(冰醋酸与水的体积比为9∶1)和     

Synthesis and electrospray ionization mass spectra of AZT/d4T boranophosphates

New anti-HIV prodrugs, conjugates of AZT and d4T with boranophosphates, were prepared by the H-phosphonate method. Their structures were determined by negative ion electrospray ionization mass spectrometry (ESI-MS) in conjunction with tandem mass spectrometry (MS/MS). The fragmentation pathways were investigated, and most of the fragment ions contained the boranophosphate or phosphinate group.     

用^3HNMR波谱法分析微波激发催化交换制备的^3H标记颠茄类生物碱

用~3H NMR波谱法测定了微波激发催化交换制备的四种~3H标记颠茄类生物碱示踪剂的氚标记位置及其相对百分含量。并在用~1H NMK归属原料纯度及标记物分子各基因化学位移时采用了水峰抑制技术(简称WEFT),既能同时消除溶剂氘代甲醇及水峰的影响;又能提高灵敏度(近10倍),从而计算出所得标记产物的化学纯度值与放化纯度值。为快速、准确寻找制备标记生物碱的最佳实验条件和控制标记物质量提供了唯一的物理无损分析方法。     

甲基丙烯酸甲酯光引发聚合中的初级自由基终止效应

本文研究了甲基丙烯酸甲酯在30℃时的光引发聚合。当光强较强时,聚合速率和光强的平方根不呈线性关系,聚合速率略低于经典动力学关系式所预示的数值。粘均聚合度的倒数和聚合速率也不呈线性关系。在考虑了初级自由基的终止反应后,这些偏离都得到了合理的解释。 比较甲基丙烯酸甲酯在30℃的光引发聚合和在60℃的过氧化苯甲酰引发聚合的数据,可以看出,初级自由基的终止效应在低温时更为重要。     

高效前沿分析的发展及在药物-蛋白结合研究中的应用

介绍了高效前沿分析方法的原理、特点、种类，综述了它在药物与蛋白结合研究中的应用及国内外研究概况；通过与高效液相色谱／前沿分析比较，阐明了毛细管电泳／前沿分析在药物蛋白结合研究中的优势；分析了在药物与蛋白结合研究中所采用的各种研究方法，通过与这些研究方法的比较，阐明了高效前沿分析的优越性及其广阔的应用前景，同时提出了在高效前沿分析方法中有待完善和注意的问题。     

Interaction between sodium tanshinone IIA sulfonate and the adriamycin semiquinone free radical: A possible mechanism for antagonizing adriamycin-induced cardiotoxity

Adriamycin (ADR) is a powerful and widely used antitumor drug, but its dose dependent cardiotoxicity limits its application. This side effect is believed to be caused by the adriamycin semiquinone free radical (ASFR). The primary focus of this work is to test effects of sodium tanshinone IIA sulfonate (STS) on ASFR and adriamycin–induced lipid peroxidation. It was found that ADR, whether in the system of heart homogenate, heart mitochondria or heart submitochondria, with NADH as the substrate or in xanthine/xanthine oxidase under anaerobic conditions, all produced ASFR rapidly. STS was shown to effectively scavenge ASFR in all these systems and postpone the appearance of ASFR. The delayed time was proportional to the amount of STS. Under aerobic conditions, ASFR could be oxidized to generate oxygen free radicals. STS could not scavenge these oxygen free radicals, but it could effectively scavenge lipid free radicals generated from membrane lipid peroxidation of heart mitochondria. STS could significantly reduce mitochondrial swelling and lipid peroxidation induced by ADR. Animal experiments show that treatment of STS could inhibit endogenous lipid peroxidation caused by ADR. Here, a protective mechanism of STS is suggested that STS can rapidly and univalently oxidize ASFR, causing the cycle of adriamycin between its quinone form and semiquinone form and inhibiting the accumulation of ASFR. Under aerobic condition, STS can protect heart mitochondria by scavenging lipid free radicals generated from adriamycin-induced mitochondrial lipid peroxidation. This investigation shows that STS may be a physiological drug to antagonize the cardiotoxicity of ADR.