表面活性剂阴离子双水相新体系及其对卟啉、染料的萃取

由阴阳离子型表面活性剂水溶液混合形成的双水相［１,２］是水相分离技术中的一个新分支．ＺＨＡＯ等［２］将阴阳离子表面活性剂过量的体系分别称为阴阳离子双水相．由溴化十二烷基三乙铵（Ｃ１２ＮＥ）和十二烷基硫酸钠（ＳＤＳ）组成的阳离子双水相对蛋白质［１］、酶［３］、氨基酸［４］和卟啉［５,６］等的萃取分离已有报道．与阳离子双水相比较,阴离子双水相分相时间慢,其萃取应用研究尚未见报道．本文在详细研究了ＳＤＳ－Ｃ１２ＮＥ阴离子双水相的基础上,将全氟型阴离子表面活性剂全氟辛酸钠（ＳＰＦＯ）引入这类水相分离体系…     

水溶性铑－膦配合物催化1－十二碳烯常压氢甲酰化反应研究

本文研究了水溶性铑配合物ＲｈＣｌ（ＣＯ）（ＴＰＰＴＳ）２在常压（ＣＯ：Ｈ２＝１：１）条件下对１－十二碳烯氢甲酰化反应的催化性能，并对催化剂浓度、表面活性剂浓度、溶液ｐＨ值、膦铑比、溶剂等因素的变化对催化活性的影响作了考察．结果表明，表面活性剂（ＣＴＡＢ）的加入，可以在反应体系中形成胶束．加速有机相和水相间的传质速度，从而提高催化转化速度．在反应温度（８０℃）下，ＣＴＡＢ的临界胶束浓度（ＣＭＣ）较室温下高．达到最佳催化活性的ｐＨ范围为７～９，［Ｐ］／［Ｒｈ］比为１６，而有机溶剂的加入则使转化数降低．     

混合反胶束的电导与微结构研究

反胶束是两亲分子在非极性溶剂中形成的一种有序组合体，在医药、化工、采油、胶束催化及酶催化等领域中有重要应用．与胶束溶液相比，人们对反胶束的形成与结构的了解至今仍不充分．特别是对于由混合表面活性剂形成的反胶束的研究几乎无人涉及．本文采用动态光散射、电导及荧光光谱等手段对阴离子表面活性剂AOT与非离子表面活性剂形成的混合反胶束进行了研究，旨在探讨利用表面活性剂的复配来调节和控制反胶束的结构和性能．亚实验部分二异辛基磺化琉璃酸钠（AOT，Sigma公司）；Brij30为含4个氧乙烯基（EO基）的十二碳醇（AcrosOrgani…     

不同添加物对表面活性剂溶液预胶束形成的影响

关于表面活性剂溶液中预胶束的形成问题已有不少报道［’－‘］．预胶束是表面活性剂溶液在浓度很稀时（远小于其临界胶束浓度（CMC》、表面活性分子所形成的一种集合体·由于一般的物理化学方法对其难于捡出，因此常被研究者忽略．文献间曾指出：预胶束形成的驱动力与胶束一样，也是疏水作用所致．因此表面活性分子的链长、头部极性、溶剂性质以及添加物的引入等因素必然会影响预胶束的形成．本工作是对添加物的引入问题所作的初步研究·。作中所研究的阴离子表面活性剂有十二烷基硫酸钠（sss）·＋”烷基；Iv酸钠（5％）和十六烷基硫酸…     

电解质水溶液在丙酸十二铵-四氯化碳溶液中的增溶

表面活性剂在非极性溶剂中形成的反胶束在催化反应、光化学、蛋白质苹取分离等方面有着广泛的应用问．这些应用与反胶束的性质有着密切的关系，而增溶水后的反胶束其形状和大小都会发生很大的变化．增溶不同水量的反胶束的微极性、酸碱性、微勤度等已有不少文献报导［2－5］．一些不溶于非极性溶剂而溶于水的物质可以溶解在非极性溶剂中的反胶束核心水团中，这个现象被称为二次增溶．其中，电解质的二次增溶对于研究配体转换反应。酶催化反应问及改变反胶束内部的微环境有着十分重要的作用，Aebi和Weibush回首先研究了有水存在时N。CI在A…     

聚乙二醇对振荡反应的影响

前文［1］曾指出，生物体系的化学振荡反应实际上是产生于水溶胶之中（包括高分子溶液及表面活性剂溶液）．作为反应介质，水溶胶对生物体系的周期现象有着不可忽略的重要作用．因此，要模拟生物体系的化学振荡就不能不考虑溶胶对振荡反应的影响．前文［2，3］报道了表面活性剂TritonX－100（简称TX－100），TritonX－305等对振荡反应的影响．为了解聚乙二醇类表面活性剂中EO链的作用及高分子溶液对振荡反应的特征影响，我们选用高分子聚乙二醇（PEG）作为添加剂，考虑由于它的加入而引起振荡反应的变化．为了减少PEG中自由羟基的还原…     

混合表面活性剂的表面活性及加溶能力

阴阳离子混合表面活性剂具有很高的表面活性［1］，但该类表面活性剂的浓度超过临界胶团浓度（cmc）以后，就将沉淀而失去表面活性［2］．因此，对该类体系的研究，主要在cmc以下．曾作过许多努力，希望解决阴阳离子混合表面活性剂的沉淀（或分层）问题，但效果均不理想［3，4］．直到最近，在这方面的研究才取得明显的进展，找到了在水溶液中，任何浓度和混合比之下，都不沉淀或分层的一类阴阳离子混合表面活性剂［4］．本文在此基础上，研究了该类表面活性剂的表面活性及其对戊醇和乙烷的加溶，该方面的研究工作，在国内外尚属首次，这对…     

荧光探针法测定甜菜碱cmc的研究

荧光探针法测定甜菜碱ｃｍｃ的研究任学贞，李干佐，王弘立，翟立民，隋卫平，徐欣艳（山东大学化学系，济南，２５０１００）关键词甜菜碱，芘，临界胶束浓度Ｅｋｗａｌｌ等［１］发现，表面活性剂的溶液能够增溶多环芳烃并发射较强的荧光．在常用的测定表面活性剂临界胶...     

电导率法测定表面活性剂的临界胶束浓度

电导率法测定表面活性剂的临界胶束浓度邹耀洪（常熟高等专科学校化学系江苏２１５５００）物化实验中测定表面活性剂临界胶束浓度（ＣＭＣ）常用表面张力法［１］，但精确测定表面活性剂水溶液的表面张力受到一些限制，如毛细管升高法中要准确地测定毛细管的半径、溶液的...     

1-(4-磺酸基苯基)-3-[4-(苯基偶氮)苯基]-三氮烯与季铵盐型阳离子表面活性剂的显色反应及应用

合成了１－（４－磺酸基苯基）－３－［４－（苯基偶氮）苯基］－三氮烯（ＳＰＡＰＴ）,研究了该试剂在强碱性介质中与季铵盐型阳离子表面活性剂溴化十六烷基吡啶（ＣＰＢ）和溴化十六烷基三甲铵（ＣＴＭＡＢ）的显色反应体系,试剂与表面活性剂形成１∶３的紫红色离子缔合物,其表观摩尔吸光系数分别为１．６７×１０４和１．０６×１０４Ｌ·ｍｏｌ－１·ｃｍ－１。测定了显色体系中ＣＰＢ和ＣＴＭＡＢ的临界胶束浓度（ＣＭＣ）,证明在比尔定律范围内,ＣＰＢ和ＣＴＭＡＢ均以单分子缔合显色。确定了显色体系最佳实验条件     

核糖核酸酶A在DAB-环乙烷溶液中的活性和构象

The activity and conformation of ribonuclerse A (RNaseA) solubilized in cyclohexane via dodecylammonium butyrate(DAB) reverse micelles were investigated. The activity of RNaseA was studied using the cytidine 2’,3’ -phosphate as the substrate, and it was found that kcat increases significantly with respect to that in water attended by an increased Km•FT-IR spectra of RNaseA in reverse micellar solution were investigated as a function of w0(= [H2O]/ [DAB]), and it was noted that the structure of RNaseA became losser in reverse micelles campared to that in aqueous solution. The relation between activity and conformation was discussed.     

核糖核酸酶A在丁酸十二铵-环己烷反胶束溶液中的催化动力学

研究了核糖核酸酶A(RNaseA)在丁酸十二铵(DAB)-环己烷反胶束溶液中催化水解胞苷2',3'-环单磷酸酯的动力学,数据符合Michaelis-Menten酶催化机理.以k_cat/K_m表示酶催化活性时,Rnase A在反胶束溶液中的催化活性是在水溶液中的14～30倍.无论是固定DAB浓度还是固定H₂O与DAB浓度之比,随增溶水量的增加,k_cat/K_m呈下降趋势.     

盐酸胍对反胶束中RNase A活性的影响

以胞嘧啶核苷酸2',3'-环单磷酸酯为底物研究了变性剂盐酸胍对十二胺丁酸盐-环己烷反胶束溶液中核糖核酸酶A活性的影响,同水溶液相比,盐酸胍对反胶束中酶活性的抑制作用很小。反胶束的大小限制了酶分子天然态构象的改变,从而保证了其活性中心的完整性。核糖核酸酶A的内源荧光研究发现,同水溶液相比,反胶束中蛋白的最大发射波长没有发生变化,但荧光偏振极化度增加,也表明了在反胶束中酶分子的运动自由度较在水溶液中有所降低。     

脂肪酸十二烷基铵在四氯化碳中的聚集行为

通过碘光谱法和对水的增溶研究了乙酸十二烷基铵(DAA)、丙酸十二烷基铵(DAP)和丁酸十二烷基铵(DAB)在四氯化碳中的聚集作用; 碘光谱测得的(cmc)~I约比水增溶法测得的(cmc)~W低一个数量级。可能因为碘光谱法测得的是开始发生聚集时的cmc, 这时聚集体较小, 对水无增溶能力; 只有当聚集体随浓度升高而长大到一定程度时, 才能开始增溶水。实验表明, DAA, DAP和DAB的反胶束对水的饱和增溶能力, 分别相当于每一个表面活性分子增溶4.2, 9.4和13.5个水分子。根据球型反胶束模型, 计算了反胶束聚集数、捕集水团的半径和自由水团的半径。     

Synthesis and further reactivity studies of some transition metal gallyl complexes

Reactions of the anionic gallium(I) heterocycle salt, [K(tmeda)][Ga(DAB)] (DAB = {N(Dip)C(H)}₂; Dip = C₆H₃Prⁱ₂-2,6), with a series of groups 6-9 and 11 metal halide complexes have given rise to the metal gallyl complexes, [CpCr(IMes){Ga(DAB)}] (IMes = :C{(Mes)NC(H)}₂; Mes = mesityl), [M(tmeda){Ga(DAB)}₂] (M = Mn, Fe or Co) and [Cu(dppe){Ga(DAB)}] (dppe = 1,2-bis(diphenylphosphino)ethane). The majority of the complexes have been crystallographically characterized. The reactivity of the previously reported copper(I) gallyl complex, [(IPr)Cu{Ga(DAB)}] (IPr = :C{(Dip)NC(H)}₂), towards a variety of unsaturated substrates has been explored. Three crystallographically characterized complexes have arisen from this phase of the study, viz. [(IPr)CuCCPh], [(IPr)Cu{Ga(DAB)}(CNBu^t)] and [(IPr)Cu{κ¹-OC(O)C(CNHDip)(NHDip)}]. The results of these investigations show that the reactivity of [(IPr)Cu{Ga(DAB)}] is significantly different to that of related copper boryl complexes.     

Synthesis of bis(cyclopentadienyl)diazadiene complexes of ytterbium. An X-ray structural study of the Cp2Yb(μ-η2:Ti2-But-N=CH-CH=N-But)Li(DME) complex

Ytterbium complexes, Cp₂Yb(-₂:²-DAB)Li(DME) (1) and CpYb(DAB)K(THF)₂ (2), containing a bridging diazadiene ligand were prepared by the reaction of CpYbCl₂(THF)₃ with (DAB)Li₂ (11) and (DAB)^–K⁺ (12) (DAB = Bu^t-N=CH-CH=N-Bu^t). The structure of complex1 was established by X-ray diffraction analysis. The complex is binuclear: the Yb atom of the Cp₂Yb fragment and the Li atom, which is bonded as well with the chelating DME molecule, are linked by the DAB ligand.Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 1, pp. 148–151, January, 1994.     

水溶性有机物与细胞膜的结合作用

以二氨基蓝3R (DAB)和玫瑰红B (RB)两种离子型有机物为探针, 研究了其与体外单层磷脂膜(SPM)和大肠杆菌之间的相互作用, 结合作用符合Langmuir和Temkin等温化学吸附方程. 考察了pH、离子强度和温度对吸附作用的影响, 分析了DAB, RB与SPM和细胞的结合形式、结合键和结合位置. 结果表明, DAB, RB与SPM和细胞外膜有强烈的单分子层化学吸附, 是自发的放热反应, 主要通过电荷对吸引、氢键等非共价键结合在SPM和细胞外表面, 且绝大部分DAB, RB积累、滞留在细胞膜壁上. 混合作用时, 两种有机物存在竞争吸附结合现象.     

The inclusion compound of emulsified cetostearyl alcohol withβ-cyclodextrin and a competitive reaction with a hydrocortisone/β-cyclodextrin inclusion compound in an oil-in-water cream

-cyclodextrin can form a solid inclusion compound with emulsified cetostearyl alcohol (ECA) by coprecipitation. This was proved by differential scanning calorimetry (DSC), X-ray diffractometry, IR spectrometry and the determination of the foaming ability according to the German Pharmacopeia (DAB 10) for ECA in the coprecipitate. The DSC result shows that both ingredients, cetostearyl alcohol and cetostearyl sulfate, are included in the-CD cavity. The coprecipitate is therefore a mixture of inclusion compounds. ECA as a constituent of Hydrophilic Ointment (DAB 10) can substitute up to 10% hydrocortisone in Aqueous Hydrophilic Ointment(DAB 10) containing 1% HC as-CD inclusion compound under the conditions of preparation.     

Computational insights into uranium complexes supported by redox-active α-diimine ligands

The electronic structures of two uranium compounds supported by redox-active α-diimine ligands, ((Mes)DAB(Me))(2)U(THF) (1) and Cp(2)U((Mes)DAB(Me)) (2) ((Mes)DAB(Me) = [ArN═C(Me)C(Me)═NAr]; Ar = 2,4,6-trimethylphenyl (Mes)), have been investigated using both density functional theory and multiconfigurational self-consistent field methods. Results from these studies have established that both uranium centers are tetravalent, that the ligands are reduced by two electrons, and that the ground states of these molecules are triplets. Energetically low-lying singlet states are accessible, and some transitions to these states are visible in the electronic absorption spectrum.     

Surface-induced dissociation of singly and multiply protonated polypropylenamine dendrimers

The ease of fragmentation of various charge states of protonated polypropylenamine (POPAM) dendrimers is investigated by surface-induced dissociation. Investigated are the protonated diaminobutane propylenamines [DAB(PA)n] DAB(PA)8 (1+ and 2+), DAB(PA)16 (2+ and 3+), and DAB(PA)32 (3+ and 4+). These ions have been proposed to fragment by charge-directed intramolecular nucleophilic substitution (SNi) reactions. Differences in relative fragment ion abundances between charge states can be related to the occupation of different protonation sites. These positions can be rationalized based on estimates of Coulomb energies and gas-phase basicities of the protonation/fragmentation sites. The laboratory collision energies at which the fragment ion current is approximately 50% of the total ion current were found to increase with the size, but to be independent of charge state of the protonated POPAM dendrimers. It is suggested that intramolecular Coulomb repulsion within the multiply protonated POPAM dendrimers selected for activation does not readily result in easier fragmentation, which is in accordance with the proposed fragmentation mechanism.