手性胶束中的有机反应(Ⅴ)——手性胶束中查耳酮的不对称环氧化

本文报道查耳酮用H₂O₂在手性表面活性剂N,N-二甲基-N-十二烷基麻黄素澳化铵(1a)及N,N-二甲基-N-十六烷基麻黄素溴化铵(1b)形成的手性胶柬水溶液中的不对称环氧化反应,得到相应的手性α,β-环氧酮,对映体过量为5～8%.     

双烃链正,负离子表面活性剂复合物水溶液的表面化学性质研究

本文研究了具有双烃链的正、负离子表面活性剂混合水溶液的表面和液相性质、。负离子表面活性剂是琥珀酸二己酯磺酸钠[简写为(C6)2SNa],正离子表面活性剂是氯化二正辛基羟乙基甲基铵[(C8)2NCl]和氯化辛基羟乙基二甲基铵[C8NCl]。为了增加复合物的溶解度,在铵基上引入了羟乙基。测定了表面张力-浓度关系,用GIBBS公式计算表面吸附量和吸附分子面积。结果表明,由于正、负表面活性离子之间的强烈相互作用,所研究的两种混合物体系的表面活性远高于单独的表面活性剂。在等摩尔混合和离子强度0.1mol/kg情况下,(C6)2SNa-(C8)2NCl体系的吸附层组成是对称的(摩尔比为1:1),且在临界胶团浓度(cmc)以上析出新相,表明此cmc实质上是复合物的溶解度;而(C6)2SNa-C8NCl体系的吸附层为不对称组成(摩尔比非1:1),在cmc以上可能形成相当大的胶团,两种体系混合溶液的起泡性有极大差异。     

AEOT/异辛烷/水反胶团体系对血红蛋白的提取

自Riet等报道以反胶团技术提取蛋白质以来,有关反胶团技术提取生物活性物质的报道较多,但研究对象多为分子量较小的蛋白质及酶.由表面活性剂丁二酸二(2-乙基己基)酯磺酸钠(AOT)形成的反胶团体系水含量W₀,有机相中水的摩尔浓度与表面活性剂摩尔浓度之比)较小,提取率偏低.     

胶束模拟酶的研究——1.手性胶束中酮的不对称还原

在( )和(-)-N-十六烷基—N,N-二甲基-α-苯乙铵溴化物(1a和1b)及N-十二烷基-N,N-二甲基麻黄素溴化铵(2)等表面活性剂形成的手性胶束溶液中,以NaBH_4还原潜手性的苯基烷基酮可诱导出不对称中心,生成旋光性的醇。e.e.%最大值可达8.6%。产物醇的构型取决于所用胶束的构型,对只有一个手性中心的胶束1a和1b,产物构型和胶束相反。手性胶束结构对产物的光学得率影响较大。     

表面胶团修饰电极电化学测定双酚A的增敏机理及抗污性能研究

分别以2种阴离子表面活性剂(SDS、SDBS)、3种季铵盐阳离子表面活性剂(CTAB、TTAB、DTAB)和2种季铵盐型双子表面活性剂(12-3-12、12-4-12)修饰碳糊电极。通过原子力显微镜、接触角以及分析物在电极表面的电化学行为探讨了不同表面活性剂在电极表面的吸附情况,推测在浓度大于临界胶束浓度(CMC)时,季铵盐型阳离子表面活性剂CTAB、TTAB、12-3-12和12-4-12在碳糊电极表面形成了圆柱形的表面胶团,而DTAB和SDS可能是饱和单分子层吸附。以BPA为分析物,研究了表面活性剂修饰电极对BPA的电化学增敏机理,结果表明修饰电极对双酚A(BPA)的电化学增敏作用主要是因为表面胶团对BPA的增溶作用,表面活性剂和BPA间的阳离子-π作用是表面胶团增溶BPA的主要原因。     

胶束模似酶的研究1.手性胶束中酮的不对称还原

在(+)和(-)-N-十六烷基-N,N-二甲基-α-苯乙铵溴化物(1a和1b)及N-十二烷基-N,N-二甲基麻黄素溴化铵(2)等表面活性剂形成的手性胶束溶液中,以NaBH~4还原潜手性的苯基烷基酮可诱导出不对称中心,生成旋光性的醇.e.e.%最大值可达8.6%.产物醇的构型取决于所 用胶束的构型,对只有一个手性中心的胶束1a和1b,.产物构型和胶束相反.手性胶束结构对产物的光学得率影响较大.     

手性胶束的不对称诱导作用不对称苯偶姻缩合反应

胶束体系是模拟酶的简单模型之一。手性胶束对反应有手性诱导作用。在表面活性剂(1R，2S)-(-)-N-十二烷基-N-甲基麻黄素溴化物和(1R，2S)-(-)-N-十六烷基-N-甲基麻黄素溴化物形成的胶束体系中进行的苯偶姻缩合反应，生成了光学活性的α-羟基酮。     

C12-s-C12·2Br和C12En混合水溶液的胶团化行为

季铵盐二聚表面活性剂C12-s-C12@2Br(s=2、3、4、6)和非离子表面活性剂C12E10或C12E23在水溶液中生成混合胶团.其临界胶团总浓度cmcT值介于二元复配体系中各组分的临界胶团浓度和之间.当添加少量非离子型表面活性剂(在水溶液中的摩尔分数α2=0.1)时,混合胶团中C12E10或C12E23的摩尔分数均已超过0.35;随着溶液中非离子型表面活性剂含量的增大,混合胶团中逐渐以C12E10或C12E23成分为主.     

C_(12)-s-C_(12)·2Br和C_(12)E_n混合水溶液的胶团化行为

季铵盐二聚表面活性剂C12-s-C12·2Br(s=2、3、4、6)和非离子表面活性剂C12E10或C12E23在水溶液中生成混合胶团.其临界胶团总浓度cmcT值介于二元复配体系中各组分的临界胶团浓度cmc01和cmc02之间.当添加少量非离子型表面活性剂(在水溶液中的摩尔分数α2=0.1)时,混合胶团中C12E10或C12E23的摩尔分数均已超过0.35;随着溶液中非离子型表面活性剂含量的增大,混合胶团中逐渐以C12E10或C12E23成分为主.     

稳态荧光探针法研究对-烷基-苄基聚氧乙烯醚羧酸甜菜碱的聚集行为

利用荧光探针法和表面张力法测定了一类疏水基中含有苯基的新型甜菜碱两性离子表面活性剂对-烷基-苄基聚氧乙烯醚羧酸甜菜碱(ABECB)的临界胶团浓度(cmc)、胶团微极性和表面张力(γ_cmc).研究结果表明,荧光探针(芘)法可用来测定这类表面活性剂的临界胶团浓度(cmc),且测定结果与表面张力法(吊片法)接近;ABECB具有较低的cmc和γ_cmc值,表明此类表面活性剂具有优良的表面活性; 胶团的微极性随着疏水链长的增大而略微减小,氧乙烯(EO)单元数的增大对ABECB胶团核内的微极性影响不明显.     

光学活性α-取代(2-吡啶基)甲胺的对映选择性合成

以2-羟基蒎烷-3-酮为手性助剂, 与2-氨甲基吡啶缩合得到中间体酮亚胺, 经去质子化、不对称烷基化、转胺反应得到光学活性α-取代(2-吡啶基)甲胺, 对映体过量值为89-98%。并提出了过渡态模型, 对对映选择性合成反应作了较为合理的解释。     

Enantiomer separation of drugs by micellar electrokinetic chromatography using chiral surfactants

A review surveying enantiomer separations by micellar electrokinetic chromatography (MEKC) using chiral surfactants is described. MEKC is one of the most popular techniques in capillary electrophoresis, where neutral compounds can be analyzed as well as charged ones, and the use of chiral micelles enable one to achieve the enantioseparation. The chiral MEKC systems are briefly reviewed according to the types of chiral surfactants along with typical applications. As chiral micelles or pseudostationary phases in MEKC, various natural and synthetic chiral surfactants are used, including several low-molecular-mass surfactants and polymerized surfactants or high-molecular-mass surfactants. Cyclodextrin modified MEKC using chiral micelles is also considered.     

昆虫性信息的结构鉴定与合成 XXVII: (5R, 6S)-(-)-及(5S, 6R)-(+)-淡色库蚊产卵引诱性信息素的立体选择性合成与手性亚砜不对称加成的立体化学

从R-(-)-正十三烯-3-醇2所得的R-(+)-醛5, 与R-(+)亚砜化合物6的不对称醇醛缩合得7a和7b(30:1). 7a经一系列转化得1a, 从(5S, 6R)-14出发, 经两次构型翻转[5S,6R)-15→(5S, 6S)-16和(5S, 6S)-17→(5R, 6S)-14], 得1a的对映体1b. 光学活性α-苄氧基醛5与手性亚砜的不对称醇醛缩合, 受手性亚砜的1,3-不对称诱导控制, 而不是受醛5的1,2-不对称诱导控制.     

胶团噻唑衍生物对安息香不对称合成反应的催化作用

通过α-(1-萘基)-N-硫代甲酰乙胺与卤代酮反应制得六个光学活性的4-烷基-3-α-(1-萘基)乙基噻唑溴化物烷基碳链长=1,2,7.11,15,21). 将其用于催化水溶液中的安息香缩合反应, 所得产物收率约20-30%具有较高的光学纯度(47-57%). 在各种缓冲溶液中测定了S(+)-4-甲基-3-α-(1-萘基)乙基噻唑氯化物(Ta)的胶团性质和由它催化的不对称安息香缩合反应. 临界胶团浓度(cmc)证明(Ta)在反应中确以胶团形式催化. 在硼砂溶液中, 安息香的收率高达61%, 光学纯度23.6%.     

光学活性姜黄烯化合物的立体选择性合成

本文报道了在手性膦过渡金属配合物催化下,以对溴甲苯与6-甲基-5-庚烯-2-溴化镁(5)经不对称交叉偶联反应合成(R)-(-)-和(S)-(+_)-α-姜黄烯的方法,光学收率分别为44%e.e和50.3%e.e.(R)-(-)-α-姜黄烯经Birch还原得到(R)-(-)-β-姜黄烯.对溴苯甲醚经不对称交叉偶联、Birch还原等反应合成了(S)-(+)-γ-姜黄烯.     

以(+)-樟脑缩苄胺作中间体对映选择合成(R)-α-取代苄胺

本文报道以(+)-樟脑作手性助剂, 苄胺为原料, 二者缩合制得的酮亚胺作中间体3,不对称合成(R)-α-取代苄胺(7)的一条有效新途径。化合物3用丁基锂去质子化提供的锂衍生物4和卤代烷反应, 以较高立体选择性产生烷基化产物6, 化合物6用醋酸羟胺转氨反应后, 获得了光学产率为4.6-90%的(R)-α-取代苄胺(7), 以肟的形式回收(+)-樟脑。     

Cubane-type Fe4S4 clusters with chiral thiolate ligation: formation by ligand substitution, detection of intermediates by 1H NMR, and solid state structures including spontaneous resolution upon crystallization

Cubane-type clusters [Fe(4)S(4)(SR*)(4)](2-) containing chiral thiolate ligands with R* = CH(Me)Ph (1), CH(2)CH(Me)Et (2), and CH(2)CH(OH)CH(2)OH (3) have been prepared by ligand substitution in the reaction systems [Fe(4)S(4)(SEt)(4)]/R*SH (1-3, acetonitrile) and [Fe(4)S(4)Cl(4)](2-)/NaSR*(3, Me(2)SO). Reactions with successive equivalents of thiol or thiolate generate the species [Fe(4)S(4)L(4-n)(SR*)(n)](2-) (L = SEt, Cl) with n = 1-4. Clusters 1 and 2 were prepared with racemic thiols leading to the possible formation of one enantiomeric pair (n = 1) and seven diastereomers and their enantiomers (n = 2-4). Reactions were monitored by isotropically shifted (1)H NMR spectra in acetonitrile or Me(2)SO. In systems affording 1 and 2 as final products, individual mixed-ligand species could not be detected. However, crystallization of (Et(4)N)(2)[1] afforded 1-[SS(RS)(RS)] in which two sites are disordered because of occupancy of R and S ligands. Similarly, (Et(4)N)(2)[2] led to 2-[SSSS], a consequence of spontaneous resolution upon crystallization. The clusters 3-[RRRR] and 3-[SSSS] were obtained from enantiomerically pure thiols. Successive reactions lead to detection of species with n = 1-4 by appearance of four pairs of diastereotopic SCH(2) signals in both acetonitrile and Me(2)SO reaction systems. Identical spectra were obtained with racemic, R-(-), and S-(+) thiols, indicating that ligand-ligand interactions are too weak to allow detection of diastereomers (e.g., [SSSS] vs [SSRR]). The stability of 3 in Me(2)SO/H(2)O media is described.     

Molecular recognition by chiral cationic micellar and micelle-like aggregates in electrokinetic capillary chromatography

We examined the enantiomer separation with micelles and a micelle-like polymer made with trimethylammonium-terminated surfactants all of whose hydrocarbon chains contain hydrogen bonding valinediamide moieties in electrokinetic chromatography (EKC). The surfactants used were 3-(N-dodecanoyl-L-valylamino)-propyltrimethylammonium bromide (surfactant 1) and 6-(N-nonanoyl-L-valylamino)hexyl-trimethylammonium bromide (surfactant 2); the micelle-like polymer was derived from 3-(N-10-undecenoyl-L-valyl)aminopropyltrimethylammonium bromide (surfactant 3). N-Acylamino acids and their isopropyl esters were separated with enantiomers with the same configuration as the chiral surfactant and which were retained to a greater extent than the counterparts in micelles. The micellar hydrophobic environment, in which amides function as hydrogen bonding sites with solutes, and ceased micellar kinetic association-dissociation with polymerization are discussed.     

Organic reactions in chiral micelles: 7. The structural effects on the asymmetric oxidation of prochiral sulfides in chiral micelles

A variety of phenyl alkyl sulfides were oxidized enantioselectively with NaIO₄ in chiral micellar systems formed from eight chiral surfactants, to give optical active sulfoxides. The enantiomer excesses ranged from 1.6 to 15.0%. To understand the mechanistic detail of this asymmetric oxidation in chiral micelle, the effects of structure both in substrates and surfactants on the optical yield of the oxidation were studied and discussed. Generally, increasing the alkyl chain length both in surfactants and in substrates enhances the optical yield, also the surfactant with hydroxy group at its appropriate position gives better enantioselectivity, suggesting the enzymic characteristics of the chiral micelle.     

Molecular recognition with micellar and micelle-like aggregates in aqueous media

In this article, attention is directed to molecular recognition by micellar aggregates made with ionic surfactants involving directed interactions of substrates. Particular emphasis is placed on chiral recognition of enantiomers by hydrogen bonding functionalities incorporated in hydrophobic micellar interior. Hydrophobic properties within micelles, the ordering of their polar headgroups containing chiral functionalities essential for the recognition and the cessation of micellar kinetic association-dissociation with polymerization and immobilization of the surfactants on the support are discussed.