基于半刚性乳酸衍生物的单一手性配位聚合物的合成、 结构与性质

在溶剂热反应条件下, 用预先合成的乳酸衍生物(R)-H₂CBA和(S)-H₂CBA分别与含氮辅助配体(E)-1,2-二(4-吡啶基)乙烯(DPEE)和1,4-二(1H-咪唑-1-基)苯(1,4-DIB)组合, 制备出2对不同结构的单一手性配位聚合物[Cd₂((R)-CBA)₂(DPEE)(H₂O)₂]_n(1-D), [Cd₂((S)- CBA)₂(DPEE)(H₂O)₂]_n(1-L), [Cd((R)-CBA)(1,4-DIB)]·H₂O(2-D)和[Cd((S)-CBA)(1,4-DIB)]·H₂O(2-L). 其中1-D和1-L是由梯形Cd-CBA链和DPEE配体连接成的二维框架结构; 而2-D和2-L是三维超分子框架结构, 包含3种不同类型的对映手性螺旋链. 对上述化合物进行了粉末X射线衍射、 热重分析和圆二色谱分析, 并对其荧光性质进行了讨论.     

直链淀粉-三[(S)-1-苯乙基氨基甲酸酯]手性固定相拆分布地奈德对映体及其制剂含量的测定

22R-布地奈德的药物活性比22S-布地奈德的强2~3倍,开发布地奈德对映体拆分和定量分析方法,可为其药物研发及质量控制提供重要依据。目前,主要以反相C₁₈固定相对布地奈德对映体进行拆分,而采用手性固定相对其进行拆分少有报道。通过考察固定相、流动相和柱温对布地奈德对映体拆分的影响,建立了基于直链淀粉-三[(S)-1-苯乙基氨基甲酸酯]手性固定相快速拆分和检测布地奈德对映体的高效液相色谱方法,其色谱条件如下:色谱柱为Chiralpak AS-RH色谱柱(150 mm×4.6 mm, 5.0 μm),流动相为乙腈-水(45∶55, v/v),柱温40 ℃,流速1.0 mL/min,二极管阵列检测器(DAD),检测波长246 nm,进样量10 μL。在该色谱条件下,布地奈德的两个对映体得到较好拆分,22R-布地奈德和22S-布地奈德的保留时间分别6.40 min和7.77 min,分离度为4.64; 22R-布地奈德和22S-布地奈德分别在各自范围内线性关系良好,相关系数(R²)均为0.9999,检出限分别为0.05 μg/mL和0.07 μg/mL,定量限分别为0.16 μg/mL和0.20 μg/mL; 4个添加水平的样品加标回收率为102.63%~104.17%,相对标准偏差(RSD)为0.08%~0.57%(n=6)。将该方法应用于1批次4个吸入用布地奈德混悬液实际样品进行检测,22R-布地奈德和22S-布地奈德的含量分别为283.15~284.63 μg/mL和259.86~261.51 μg/mL。该方法操作简便,分析时间短,重复性好,准确度高,可用于布地奈德对映体的拆分及其制剂的质量控制。     

基于手性配体交换反应立体选择性萃取分离氧氟沙星对映体

基于配体交换反应,研究了氧氟沙星对映体在含有Cu²⁺和N-n-十二烷基-L-脯氨酸手性配体(L)两相体系中的分配平衡.在不同pH条件下,考察了Cu²⁺在含有N-n-十二烷基-L-脯氨酸两相中的分布;研究了pH,Cu²⁺浓度,手性配体浓度等因素对氧氟沙星对映体在两相中的分配系数(K)和分离因子(α)的影响.实验结果表明,N-n-十二烷基-L-脯氨酸对R-氧氟沙星对映体萃取能力大于对S-对映体的萃取能力;pH对K和α的影响很大,在pH值小于3.5时,L₂Cu二元配合物的生成在热力学上看是不适宜的,萃取时pH宜大于3.5;手性配体和Cu²⁺摩尔比为2:1,K和α最佳;使用2×1中空纤维膜对氧氟沙星对映体进行萃取分离,出口水相氧氟沙星对映体浓度比值(S/R)约为1.72.     

薤中新的甾体皂苷类化学成分

从薤(Allium chinense G. Don)的乙醇提取物中分离得到6个新甾体皂苷类化合物, 通过波谱数据及理化性质分析, 鉴定其分别为5α-cholano-22,16-内酯-3-O-β-D-吡喃葡萄糖基-(1→2)-[β-D-吡喃葡萄糖基-(1→3)]-β-D-吡喃葡萄糖基(1→4)-β-D-吡喃半乳糖苷(1)、 6-酮-5α-cholano-22,16-内酯-3-O-β-D-吡喃木糖基-(1→4)-[α-L-吡喃阿拉伯糖基-(1→6)]-β-D-吡喃葡萄糖苷(2)、 (25R)-26-O-β-D-吡喃葡萄糖基-5α-呋喃甾烷-3β,26-二醇-3-O-β-D-吡喃葡萄糖基-(1→2)-[β-D-吡喃葡萄糖基-(1→3)]-β-D-吡喃葡萄糖基(1→4)-β-D-吡喃半乳糖苷(3)、 (25R)-6-酮-26-O-β-D-吡喃葡萄糖基-5α-呋喃甾烷-3β,22α,26-三醇-3-O-α-L-吡喃木糖基-(1→4)-β-D-吡喃葡萄糖苷(4)、 (25R)-6-酮-5α-呋喃甾烷-3β,22α,24β,26-四醇-3-O-β-D-吡喃木糖基-(1→4)-[α-L-吡喃阿拉伯糖基-(1→6)]-β-D-吡喃葡萄糖苷(5)和(25R)-5α-呋甾-2α,3β,22α, 26-四醇-26-O-β-D-吡喃葡萄糖苷(6). 化合物1和2的皂苷元骨架在天然产物中首次分离得到. 选用H₂O₂诱导PC12细胞神经氧化损伤模型, 初步考察了6种新的呋甾型化合物的抗氧化活性, 实验结果表明, 化合物3对由H₂O₂诱导的细胞氧化损伤有显著的保护效果.     

具有三核Cd(Ⅱ)簇单元和螺旋链的脯氨酸类单一手性金属-有机框架材料的合成、 结构和性质

在溶剂热反应条件下, 使用含氮辅助配体1,4-二(4-吡啶基)苯(1,4-DPB)和半刚性脯氨酸衍生物配体(R)-5-(2-羧基吡咯烷-1-羰基)间苯二甲酸[(R)-H₃PIA]或(S)-5-(2-羧基吡咯烷-1-羰基)间苯二甲酸[(S)-H₃PIA]与Cd²⁺构筑了单一手性金属-有机框架材料[Cd_1.5((R)-PIA)(1,4-DPB)_1.5]·0.75H₂O·xGuest(1-D)和[Cd_1.5((S)-PIA)(1,4-DPB)_1.5]·0.75 H₂O·xGuest(1-L). 配合物1-D和1-L呈具有开放孔道的三维柱层式框架结构, 含有三核镉簇单元 Cd₃(CO₂)₆与两种螺旋链构建的波浪形Cd-PIA层. 分别对上述化合物进行了粉末X射线衍射、 热重分析、 圆二色谱和荧光光谱等测试. 测试结果显示配合物1-D和1-L都是以纯晶体的形式存在, 2种配合物的热失重曲线接近, 圆二色谱有明显的正负吸收峰, 符合其对映体的结构特征.     

红树林植物尖瓣海莲内生真菌Penicillium sp.B21次级代谢产物的分离鉴定

研究了红树林植物尖瓣海莲叶内生真菌Penicillium sp.B21次级代谢产物。 用硅胶柱层析、制备薄层层析和重结晶等方法,从该菌发酵液的乙酸乙酯萃取相中首次分离获得5个单体化合物,运用现代波谱技术、单晶X射线衍射以及文献数据对照,鉴定其结构分别为8-羟基-6甲基-1-甲氧羰基酮(1)、大黄素(2)、ω-羟基大黄素(3)、(3R,4S)-6,8-二羟基-3,4,5-三甲基-3,4-二氢异香豆素(4)和3,6,8-三羟基-3,5,7-三甲基-3,4-二氢异香豆素(5)。 首次获得了sclerotinin B单晶结构。     

共振瑞利散射法对普萘洛尔特效适配体系的手性分析

本文提出了对于手性药物普萘洛尔手性识别和手性分析的新方法。 该方法引用基于氧化石墨烯的指数富集配体系统进化筛选技术(GO-SELEX),经过10轮优化筛选出对心血管药物普萘洛尔有高度亲和力的特效适配体。 然后通过共振瑞利散射光谱法(RRS)对反应体系进行特效性检测,实验表明S-普萘洛尔和R-普萘洛尔有迥然不同的光谱差异,S-普萘洛尔与特效适配体结合后的RRS显著增强,而R-普萘洛尔与适配体结合后的RRS几乎没有变化。 据此可以对心血管药物手性普萘洛尔进行有效的手性识别。 在考察反应体系和实验条件的基础上,可对S-普萘洛尔进行实验检测,同时对外消旋体中的R-普萘洛尔进行计算分析。 实验对S-普萘洛尔的线性范围为5~275 nmol/L,检测限为0.5 nmol/L。 方法应用于外消旋药片的分析检测,结果令人满意。 实验表明,RRS检测特效适配体结合的手性靶标体系会彰显不同的光谱差异,从而可对手性对映体进行手性识别,尤其是可利用其光谱差异实现同时测定的手性分析,方法可在特殊情形下不经分离而同时测定手性对映体,具有推广应用价值。     

开口箭化学成分及抗肿瘤活性

从开口箭新鲜根茎中分离得到8个化合物, 通过理化性质分析、 质谱、 红外光谱及核磁共振波谱检测等方法鉴定了其结构, 分别为开口箭皂苷J(1)、 (25S)-26-O-β-D-吡喃葡萄糖基呋甾-1β,3β,22α,26-四羟基-3-O-β-D-吡喃葡萄糖苷(2)、 洋地黄毒苷元-3-O-α-L-吡喃岩藻糖苷(3)、 弯蕊皂苷元B(4)、 异罗斯考皂苷元(5)、 罗斯考皂苷元(6)、 香豌豆酚(7)及(+)-儿茶素(8). 其中, 化合物1为新化合物, 化合物3, 4, 7和8为首次从该属植物中分离得到. 在抗人结肠癌细胞LoVo和胃癌细胞BGC-823活性评价中, 化合物5和6表现出较强的抗肿瘤活性, 半抑制浓度(IC₅₀)值分别达到0.532和0.757 μmol/L.     

手性杯[4]芳烃氨基醇的合成及自组装

用25,27-二(2-溴乙氧基)-26,28-二羟基-5,11,17,23-四叔丁基杯[4]芳烃与光学纯的(1S,2R)-(+)-2-氨基-1,2-二苯基乙醇合成了手性杯[4]芳烃氨基醇2. 2能在极性的甲醇中组装成二聚体,通过¹H NMR滴定测定其结合常数K_a为34.7 M^-1,并提出了自组装机理.     

量子化学计算解析手性共价有机框架材料6色谱固定相的手性拆分机理

为探究手性共价有机框架材料6(Chiral Covalent Organic Frameworks 6, CCOF6)色谱固定相的手性拆分机理,首先运用ORCA程序对CCOF6及4对手性对映体进行结构优化,然后使用AutoDock程序对CCOF6及各对映体分子进行分子对接,获得CCOF6与对映体相互作用的初始构型;采用ORCA程序(B3LYP泛函,带DFT-D3校正,轨道基组为def2-TZVP, def2/J作为RI-J的辅助基组,RIJCOSX用来加速计算)对初始构型进行能量计算,以最终确定CCOF6与对映体的相互作用构型,并获得相应的结合自由能和结合自由能差;使用Multiwfn程序对ORCA结果进行独立梯度模型分析,并应用视觉分子动力学程序可视化展示CCOF6与对映体的弱相互作用。结果表明:①在计算结合自由能方面,考虑了溶剂效应的ORCA计算方法比不考虑溶剂效应的ORCA以及AutoDock计算方法更为精确;②CCOF6色谱固定相与对映体之间的结合自由能差绝对值越大,对映体的选择性因子也越大,然而对映体的分离度不一定会越大;③除S-1-苯基-1-丙醇是以羟基和CCOF6的醚键发生相互作用外,其他对映体皆为羟基与CCOF6的羰基发生相互作用,且S-1-苯基-1-丙醇与CCOF6的结合力最弱;④结合对映体的出峰时间和其与CCOF6的结合自由能大小可以推断,正己烷/异丙醇流动相对1-苯基-1-丙醇的洗脱能力最弱,正己烷/异丙醇流动相对1-苯基-2-丙醇的洗脱能力次弱;⑤除了S-1-苯基-1-丙醇出峰时间迟于R-1-苯基-1-丙醇,其余对映体均为R型出峰时间迟于S型。     

Asymmetric transfer hydrogenation of ferrocenyl ketones: a new simple route to chiral ferrocenyl alcohols

The asymmetric transfer hydrogenation (ATH) of ferrocenyl ketones, such as FcC(O)CH₂Y [Fc = ferrocenyl, Y = H (1a), CH₃ (1b), Cl (1c) or N₃ (1d)] has been carried out using the Noyori/Ikariya catalysts [(−)-(1R,2S)-ephedrine] or N-tosyl-(1R,2R)-diphenylethylenediamine [(R,R)-TsDPEN] as chiral ligands combined with [RuCl₂(η⁶-benzene)]₂ and 2-PrOH or HCO₂H–Et₃N as the hydrogen sources, respectively. The best results were achieved with the [(R,R)-TsDPEN–Ru^IIHCO₂H–Et₃N] catalytic system, which produced the ferrocenylalcohols (R)-2a, (R)-2c, and (R)-2d in good yields and excellent enantiomeric excesses (>98% ee).     

Synthesis, characterization and catalytic activity in Heck-type reactions of orthometallated Pd and Pt complexes derived from (1R,2R)-1,2-diaminocyclohexane

The chiral bis-imine (1R,2R)-C₆H₁₀-[E---N=CH---C₆H₃---3,4-(OMe)₂]₂ 1 (LH) reacts with [Pd(OAc)₂] (1:1 molar ratio; OAc=acetate) giving the orthometallated [Pd(OAc)(C₆H₂---4,5-(OMe)₂---2-CH=N-(1R,2R)-C₆H₁₀---N=CH---C₆H₃-3′,4′-(OMe)₂-κ-C,N,N)] 2 (abbreviated as [Pd(OAc)(L-κ-C,N,N)]), through C---H bond activation on only one of the aryl rings and N,N-coordination of the two iminic N atoms. 2 reacts with an excess of LiCl to give [Pd(Cl)(L-κ-C,N,N)] 3. The reaction of 3 with AgClO₄ and neutral or anionic ligands L′ (1:1:1 molar ratio) affords [Pd(L-κ-C,N,N)(L′)](ClO₄) (L′=PPh₃ 4a, NCMe 5, pyridine 6, p-nitroaniline 7) or [Pd(I)(L-κ-C,N,N)] 8. Complex 4a reacts with wet CDCl₃ giving [Pd(C₆H₂---4,5-(OMe)₂---2-CH=N-(1R,2R)---C₆H₁₀---NH₂-κ-C,N,N)(PPh₃)](ClO₄) 4b as a result of the hydrolysis of the C=N bond not involved in the orthometallated ring. The molecular structure of 4b·CH₂Cl₂ has been determined by X-ray diffraction methods. Cleavage of the Pd---N bond trans to the C_aryl atom can be accomplished by coordination of strongly chelating ligands, such as acetylacetonate (acac) or bis(diphenylphosphino)ethane (dppe), forming [Pd(acac-O,O′)(L-κ-C,N)] 9 and [Pd(L-κ-C,N)(dppe-P,P′)](ClO₄) 12, while classical N,N′-chelating ligands such as 1,10-phenantroline (phen) or 2,2′-bipyridyl (bipy) behave as monodentate N-donor ligands yielding [Pd(L-κ-C,N,N)(κ¹-N-phen)](ClO₄) 10 and [Pd(L-κ-C,N,N)(κ¹-N-bipy)](ClO₄) 11. Treatment of 1 with PtCl₂(DMSO)₂ (1:1 molar ratio) in refluxing 2-methoxyethanol gives Cl₂Pt[(NH₂)₂C₆H₁₀---N,N′] 13a and [Pt(Cl)(C₆H₂---4,5-(OMe)₂---2-CH=N-(1R,2R)---C₆H₁₀---NH₂-κ-C,N,N)] 13b, while [Pt(Cl)(L-κ-C,N,N)] 14 can be obtained by reaction of [Pt(μ-Cl)(η³-2-Me---C₃H₄)]₂ with 1 in refluxing CHCl₃. Complexes 2 and 3 catalyzed the arylation of methyl acrylate giving good yields of the corresponding methyl cinnamates and TON up to 847 000. Complex 3 also catalyzes the hydroarylation of 2-norbornene, but with lower yields and without enantioselectivity.     

Synthesis of new chiral amino ether derivatives: synthetic application of meso aziridinium ions prepared from β-amino alcohols

Methods of synthesis of new chiral amino ether derivatives through the opening of aziridinium ions, prepared in situ using trans-(±)-2-(1-N,N-dialkylamino)cyclohexyl mesylate with (R)-(+)-1,1′-bi-2-naphthol, are described. The (R,R,R)-diastereomer was obtained as the major product and isolated as an enantiopure salt, and characterized by single crystal X-ray analysis. The C₂-chiral (R,R,R,R,R)-diamino ether was obtained as the major product by opening of the aziridinium ion, prepared using trans-(±)-2-(1-pyrrolidino)cyclohexyl mesylate and (R)-(+)-1,1′-bi-2-naphthol in the presence of aq NaOH. This was also characterized by single crystal X-ray analysis.     

Chiral Non-racemic Bis(vicinal 1,2-Diamines): 4,5-Diamino-N-(3,4-diaminobutyl)pentanamide Tetrahydrochloride, N,N′-Bis[3,4-bis (t-butoxycarbonylamino)butyl]urea and N,N′Bis

The reaction of (R) or (S)-N⁴,N⁵-bis(t-butoxycarbonyl)-4,5-diaminopentanoic acid (6) with (R) or (S)-N³,N⁴-bis(t-butoxycarbonyl)-3,4-diaminobutylisocyanate (8) catalyzed by 4-dimethylamino pyridine (DMAP), leads to the synthesis of (R,R), (S,S), (R,S) and (S,R) isomeric amides (11 a — d) The addition of adipic acid monomethyl ester to (R) or (S) isocyanate, followed by saponification, acidification and subsequent reaction with the second molecule of (R) or (S) isocyanate allows isolation of the (R,R), (S.S) and the meso isomers of N,N′-bis[3,4-bis(t-butoxycarbonylamino) butyl]hexanediamide (17) Removal of protecting groups with HCl/EtOH affords chiral non-racemic molecules having two free vicinal diamine units.     

Stereoselective synthesis of (1R,2S)-2-amino-1,3-diols from (R)-cyanohydrins

Vinyl substituted (1R,2S)-amino alcohols 5 were obtained by addition of vinyl magnesium bromide to the corresponding cyanohydrin O-trimethylsilyl ethers (R)-2. The O- and N-protected vinyl amino alcohols 6 were ozonized at −78°C in methanol yielding (1R,2S)-2-amino-1,3-diols7 in high enantiomeric and diastereomeric excesses. For purification, compounds 7 in some cases were acetylated to give the derivatives (1R,2S)-8. Racemic 6a was converted by oxidative ozonolysis at −78°C in methanolic NaOH solution to the corresponding methyl N-acetyl-β-hydroxy propanoate 9a. The configuration of (1R,2S)-8a was confirmed by x-ray crystallographic analysis.     

Asymmetric synthesis catalyzed by chiral ferrocenylphosphine-transition metal complexes VII. New chiral ferrocenylphosphines with C2 symmetry

A new chiral ferrocenylphosphine ligand, 2,2′-bis[1-N,N-dimethylamino)ethyl]-1,1′-bis(diphenylphosphino)ferrocene (2), which has C₂ symmetry and a functional group on the side chain, was prepared by ortho-lithiation and phosphination of 1,1′-bis[1-N,N-dimethylamino)ethyl]ferrocene followed by optical resolution; recrystallization of the diammonium salt with tartaric acid. An X-ray diffraction study of PdCl₂[(+)-2] showed that the complex has square-planar geometry with two cis chlorine and two phosphorus atoms and ligand (+)-2 has an (S) configuration on the 1-dimethylaminoethyl side chain and (R) ferrocene planar chirality.     

The synthesis and x-ray structure of (N,N-dimethyldithiocarbamato)(n-butyl)diphenyltin(IV)

(N,N-Dimethyldithiocarbamato)(n-butyl)diphenyltin(IV), n-BuPh₂SnS₂NMe₂, crystallizes in the monoclinic space group P2₁/n with a 9.772(5), b 9.895(4), c 21.418(9) Å, β 95.81(3)⁰, V 2060 ų Z = 4, μ 14.4 cm⁻¹ The structure was determined by the heavy-atom technique from 3103 independent reflections measured at room temperature on an Enraf-Nonius four-circle CAD-4 diffractometer using monochromatized Mo-K radiation and refined to a final R value of 5.8%. The tin atom is essentially four-coordinated with a weak fifth tin-sulphur bond (Sn---S(2) 3.079(1) Å) considerably longer than the other (Sn---S(1) 2.466(1) Å). A comparison with the complex n-BuPhSn(C1)S₂CNEt₂ (Sn---S(1) 2.454(1) Å; Sn---S(2) 2.764(1) Å) suggests that enhanced steric factors are responsible for the preferential monodentate behaviour of the dithiocarbamate ligand in the title complex.     

Asymmetric silyl nitronate cycloadditions with bornane-10,2-sultam derivatives

Asymmetric silyl nitronate cycloadditions with N-acryloyl (2R)-bornane-10,2-sultam, N-acryloyl (2S)-bornane-10,2-sultam, and N-methacryloyl (2R)-bornane-10,2-sultam have been studied. The asymmetric silyl nitronate cycloaddidon/elimination methodology provides a general route for the asymmetric synthesis of 2-isoxazolines.     

Dynamic behaviour and X-ray analysis of chiral η-allylpalladium complexes. II

The DANTE technique and NOESY two-dimensional method have been employed to observe the isomerization of the chiral cationic complex [Pd(η³-CH₂CMeCH₂(P-P′)]⁺ (1a), where P-P′ = the chiral chelating ligand (S)(N-diphenylphosphino)(2-diphenylphosphinoxymethyl)pyrrolidine. The rate constant was found to be 0.5 s⁻¹ in CHCl₃ at 295 K and 1.50 s⁻¹ in the presence of added free ligand. In the latter case the epimerization proceeds by a π-σ-π mechanism via the intermediacy of a primary η¹-allylpalladium complex. Although the intermediate was not detected, the NMR findings reveal that it has the allylic terminus η¹-bonded to palladium. The structure of 1a in its PF₆⁻ salt has been determined. The compound crystallizes in the orthorhombic space group P2₁2₁2₁ with a 10.029(4) b 19.203(8) c 36.115(6) Å, Z = 8, R = 0.0572 and R_w = 0.0712 for 3716 observed reflections with I > 3σ(I).     

Molecular self-assembling of chiral and racemic butan-2-ol in carbon tetrachloride solutions

The self-association of (R)-, (S)- and (RS)-butan-2-ol in their carbon tetrachloride solutions was studied through the mid-infrared (mid-IR) and near-infrared (NIR) spectroscopic observations. The mid-IR and NIR spectra for each chiral butan-2-ol were compared with those for the racemic (RS)-butan-2-ol. Although it has been reported that the hydrogen bonding among the chiral butan-2-ol molecules was stronger than that among the racemic ones, any distinguishable differences between the chiral and the racemic butan-2-ol in CCl₄ solution or even in their pure liquid state were not observed both in their mid-IR and NIR spectra. A superior analytical method, assuming a successive association process for the alcohol molecules, was applied to the analysis of the sharp band at 3630 cm⁻¹ (the OH-stretching vibration mode attributed to free OH-monomer) for the (R)-, (S)- or (RS)-butan-2-ol in CCl₄. The mean association number N for each alcohol increased with increasing in concentration until 0.12 mol dm⁻³ and then becomes constant (about four). On the other hand, Zanker's plotting method, assuming an equilibrium between monomers and only one kind of polymer species, was also applied to the analysis of the above spectroscopic results; the association number n evaluated from the Zanker's method fairly agreed with the N value in the concentration region of 0.12–0.60 mol dm⁻³.