The Williamson Reaction: A New and Efficient Method for the Alternate Resolution of 2,2'-Bis(bromomethyl)-1,1'-binaphthyl and 1,1'-Binaphthalene-2,2'-diol

Treatment of 2,2'-bis(bromomethyl)-1,1'-binaphthyl [(R,S)-2] with 1,1'-binaphthalene-2,2'-diol (+)-(R)-1 and cesium or potassium carbonate in refluxing acetone, gave the diastereoisomeric dioxacyclophanes (-)-(R,S)-3a and (+)-(R,R)-3b, both obtained in high yield, and the cyclic tetraether (+)-(R,R,R,S)-4 as isolated side product. Boron tribomide-promoted ether cleavage of 3a and 3b gave optically pure (-)-(S)-2 and (+)-(R)-2, respectively, and the recovered diol (+)-(R)-1. Alternatively, the same reaction sequence furnished the resolved diols (-)-(S)-1 and (+)-(R)-1 from (R,S)-1 and (+)-(R)-2, as well as optically pure 2,2'-bis(chloromethyl)-1,1'-binaphthyl (+)-(R)-5 from the racemic dibromide (R,S)-2 by using boron trichloride for ether cleavage.     

EPR, ENDOR, and DFT study of free radicals in L-lysine·HCl·2H2O single crystals X-irradiated at 298 K

With K-band EPR (Electron Paramagnetic Resonance), ENDOR (Electron-Nuclear DOuble Resonance), and EIE (ENDOR-induced EPR) techniques, three free radicals (RI-RIII) in L-lysine hydrochloride dihydrate single crystals X-irradiated at 298 K were detected at 298 K, and six radicals (R1, R1', R2-R5) were detected if the temperature was lowered to 66 K from 298 K. R1 and RI dominated the central portion of the EPR at 66 and 298 K, respectively, and were identified as main chain deamination radicals, (-)OOC?H(CH(2))(4)(NH(3))(+). R1' was identified as a main chain deamination radical with the different configuration from R1 at 66 K, and it probably formed during cooling the temperature from 298 to 66 K. The configurations of R1, R1', and RI were analyzed with their coupling tensors. R2 and R3 each contain one α- and four β-proton couplings and have very similar EIEs at three crystallographic axes. The two-layer ONIOM calculations (at B3LYP/6-31G(d,p):PM3) support that R2 and R3 are from different radicals: dehydrogenation at C4, (-)OOCCH(NH(3))(+)CH(2)?H(CH(2))(2)(NH(3))(+), and dehydrogenation at C5, (-)OOCCH(NH(3))(+)(CH(2))(2)?HCH(2)(NH(3))(+), respectively. The comparisons of the coupling tensors indicated that R2 (66 K) is the same radical as RII (298 K), and R3 is the same as RIII. Thus, RII and RIII also are the radicals of C4 and C5 dehydrogenation. R4 and R5 are minority radicals and were observed only when temperature was lowered to 66 K. R4 and R5 were only tentatively assigned as the side chain deamination radical, (-)OOCCH (NH(3))(+)(CH(2))(3)?H(2), and the radical dehydrogenation at C3, (-)OOCCH(NH(3))(+)?H(CH(2))(3)(NH(3))(+), respectively, although the evidence was indirect. From simulation of the EPR (B//a, 66 K), the concentrations of R1, R1', and R2-R5 were estimated as: R1, 50%; R1', 11%; R2, 14%; R3, 16%; R4, 6%; R5, 3%.     

番荔枝皂素(4S,5S)和(4S,5R)-Muricatacin的合成及Annonacin四氢呋喃段绝对构型的确证

本文以L-谷氨酸为原料合成了(1S,5S)和(4S,5R)-Muricatacin,并以该两化合物的NMR和[a]~D数据确证了Annonacin中四氢呋喃段的四个手性中心为(15R,16R,19R,20R).     

Studies on the constituents of Broussonetia species X. Six new alkaloids from Broussonetia kazinoki Sieb.

Six new alkaloids, broussonetines W, X, M1, U1, J3, and J2 (1-6) were isolated from the branches of Broussonetia kazinoki SIEB. (Moraceae) as minor constituents. They were formulated as (2R,3R,4R,5R)-2-hydroxy-methyl-3,4-dihydroxy-5-17-(cyclohexy-2-on-1(6)-enyl)heptyllpyrrolidine (1), (2R,3S,4R,5R)-2-hydroxymethyl-3,4-dihydroxy-5-17-(cyclohexy-2-on-1(6)-enyl)heptyl]pyrrolidine-4-O-beta-D-glucopyranoside (2), (2R,3R,4R,5R)-2-hydroxymethyl-3,4-dihydroxy-5-[(9R)-9,13-dihydroxytridecyl]- pyrrolidine (3), (2S,3S,4S)-2-hydroxymethyl-3,4-dihydroxy-5-(10-oxo-13-hydroxytridecyl)-5- pyrroline (4), (2R)-2-[(IS,2S)-1,2-dihydroxy-8-1(2R,3R,4R,5R)-5-(2-hydroxymethyl-3,4-dihydroxy-1-acetylpyrrolidinyl)loctyl]piperidine (5), (2R)-2-[(1S,2S)-1,2-dihydroxy-8-[(2R,3R, 4R,5R)-5-(2-hydroxymethy]-3,4-dihydroxypyrrolidinyl)]octyl]piperidine (6).     

Synthesis and characterisation of trigonal C2-chiral di- and tetra-substituted bis(oxazoline) alkyl zinc complexes and their reactivity towards protic reagents

A series of zinc(ii) alkyl complexes stabilised by the C(2)-chiral bis(oxazoline) ligand ((R(1),R(2))BOX, with R(1) = (4S)-tBu, R(2) = H (a); R(1) = (4S)-Ph, R(2) = H (b); R(1) = (4R)-Ph, R(2) = (5S)-Ph (c)), has been synthesised and structurally characterised. ((R(1),R(2))BOX)H ligands react with ZnEt(2) in toluene to give the heteroleptic three-coordinate compounds of ((R(1),R(2))BOX)ZnEt, 1a, 1b and 1c in high yield. However, when the addition of (BOX)H ligands (a-b) over ZnEt(2) is "uncontrolled", the formation of homoleptic four-coordinate compounds are favoured (2a-b), but not for the more sterically crowded ligand (c). The zinc-ethyl derivatives (1a-c) react readily with protic reagents such as acetic acid (HOAc) and methanol (MeOH). For compounds 1a-c a redistribution of ligands is observed leading preferentially to homoleptic compounds, except for the bulkier ligand c providing a three-coordinate complex identified as ((Ph,Ph)BOX)Zn(OMe), 4c. The reaction of acetylacetone (acacH) with compounds 1a-c leads straightforwardly to the more stable four-coordinate compounds corresponding to ((R(1),R(2))BOX)Zn(η(2)-acac), 5a-c. The potential of these compounds as initiators for the copolymerisation of epoxides with CO(2) was investigated.     

Insertion reactions of beta-diketiminate-stabilised calcium amides with 1,3-dialkylcarbodiimides

A series of heteroleptic beta-diketiminate-stabilised calcium amides of the form [{ArNC(Me)CHC(Me)NAr}Ca{NR(1)R(2)}(THF)] (Ar = 2,6-diisopropylphenyl; R(1) = H, R(2) = Ar; R(1) = H, R(2) = CH(2)CH(2)OMe; R(1) = R(2) = Ph) react with 1,3-dialkylcarbodiimides, R(3)N[double bond, length as m-dash]C[double bond, length as m-dash]NR(3) (R(3) = Cy, (i)Pr), to yield the corresponding insertion products [{ArNC(Me)CHC(Me)NAr}Ca{(R(3)N)(2)CNR(1)R(2)}(THF)] at room temperature in hydrocarbon solutions. These latter compounds contain both beta-diketiminate and guanidinate ligands bound to calcium. Solid-state data are consistent with the guanidinate ligands adopting a number of binding modes including kappa(2) through kappa(3) coordination, with varying degrees of delocalisation of the non-bound guanidinate nitrogen lone-pair across the pi-framework of the ligand. DFT computational studies have been conducted to address these variations in coordination behaviour.     

A new route to achiral and chiral 1,2-bis(phosphino)ethanes, 1-arsino-2-phosphinoethanes, and 1,3-bis(phosphino)propanes and the molecular structure and catalytic activity of some rhodium(I) complexes derived thereof

A series of unsymmetrical 1,2-bis(phosphino)ethanes R(2)PCH(2)CH(2)PR'(2) and 1-arsino-2-phosphinoethanes R(2)AsCH(2)CH(2)PR'(2) mainly with bulky substituents R and R' were prepared from the cyclic sulfate by stepwise cleavage of the carbon-oxygen bonds by LiPR(2) and LiPR'(2) or LiAsR(2) and LiPR'(2), respectively. Analogously, racemic mixtures of R(2)PCH(2)CH(Me)PPh(2)(R =iPr, Cy ) as well as the enantiomers (R)-, (R)- and (R)-tBu(2)PCH(2)CH(Me)PPh(2)(R)- were obtained from the corresponding unsymmetrical cyclic sulfates and (S)-. On a similar route, the racemates of the 1,3-bis(phosphino)propanes R(2)PCH(2)CH(2)CH(Me)PPh(2)(R =iPr, tBu ), optically pure (R)- and (S,S)-iPr(2)PCH(Me)CH(2)CH(Me)PPh(2)(S,S)- were prepared. The reaction of [[RhCl([small eta](4)-C(8)H(12))](2)] with chelating ligands L-L, where L-L is R(2)PCH(2)P(men)(2)(R =iPr, Ph; men =(1S,2R,5S)-menthyl), Cy(2)AsCH(2)P(men)(2), or (R)-, (R)-, (R)-, (R)- and (S,S)-, in the presence of AgPF(6), gave the complexes [Rh(eta(4)-C(8)H(12))(L-L)]PF(6) which were used as pre-catalysts in the hydrogenation of the methyl ester of alpha-acetamidocinnamic acid (ACM). Depending on L-L, the solvent, the temperature and the pressure of H(2), optical yields of up to 69% ee were achieved. For two of the rhodium complexes, and, the molecular structures were determined by X-ray crystallography.     

Salen-based chiral fluorescence polymer sensor for enantioselective recognition of α-hydroxyl carboxylic acids

(R,R)-Salen-based chiral polymer P-1 was synthesized by the polymerization of 5,5'-((2,5-dibutoxy-1,4-phenylene)bis(ethyne-2,1-diyl))bis(2-hydroxy-3-(piperidin-1-ylmethyl) benzaldehyde (M-1) with (1R,2R)-cyclohexane-1,2-diamine (M-2) via nucleophilic addition- elimination reaction, and (R,R)-salan-based polymer P-2 could be obtained by the reduction reaction of P-1 with NaBH(4). (R,R)-Salen-based chiral polymer P-1 can exhibit greater fluorescence enhancement response toward (l)-α-hydroxyl carboxylic acids, and the value of enantiomeric fluorescence difference ratio (ef) can reach as high as 8.41 for mandelic acid and 6.55 for lactic acid. On the contrary, (R,R)-salan-based chiral polymer P-2 shows obvious fluorescence quenching response toward α-hydroxyl carboxylic acids. Most importantly, (R,R)-salen-based polymer P-1 can display bright blue fluorescence color change in the presence of (l)-α-hydroxyl carboxylic acids under a commercially available UV lamp, which can be clearly observed by the naked eyes.     

Synthesis and characterization of some new C2 symmetric chiral bisamide ligands derived from chiral Feist's acid

The hemilabile chiral C2 symmetrical bidentate substituted amide ligands (1R,2R)-5(a-d) and (1S,2S)-6(a-d) were synthesized in quantitative yield from (1R,2R)-(+)-3-methylenecyclo-propane-1,2-dicarboxylic acid (1R,2R)-3 and (1S,2S)-(-)-3-methylene-cyclopropane-1,2-dicarboxylic acid (1S,2S)-3, in two steps, respectively. The chiral Feist's acids (1R,2R)-3 and (1S,2S)-3 were obtained in good isomeric purity by resolution of trans-(±)-3-methylene-cyclopropane-1,2-dicarboxylic acid from an 8:2 mixture of tert-butanol and water, using (R)-(+)-α-methylbenzyl amine as a chiral reagent. This process is reproducible on a large scale. All these new synthesized chiral ligands were characterized by 1H-NMR, 13C-NMR, IR, and mass spectrometry, as well as elemental analysis and their specific rotations were measured. These new classes of C2 symmetric chiral bisamide ligands could be of special interest in asymmetric transformations.     

Design, synthesis, and 1,3-dipolar cycloaddition of (5R)- [and (5S)]-5,6-dihydro-5-phenyl-2H-1,4-oxazin-2-one N-oxides as chiral (E)-geometry-fixed alpha-alkoxycarbonylnitrones

Optically pure (5R)- [and (5S)]-5,6-dihydro-5-phenyl-2H-1, 4-oxazin-2-one N-oxides [(5R)- and (5S)-2] were designed as chiral (E)-geometry-fixed alpha-alkoxycarbonylnitrones 1. The nitrones (5R)- and (5S)-2 were synthesized by three-step oxidation of (R)- and (S)-phenylglycinols [(R)- and (S)-3], condensation of the resulting (R)- and (S)-2-hydroxylamino-2-phenylethanols [(R)- and (S)-5] with glyoxylic acid, and cyclization of the intermediary nitrones (R)- and (S)-6b. The nitrone (5R)-2reacted with olefins 7-14 under mild conditions to afford the corresponding cycloadducts 15-22 as the main products via the least sterically demanding exo modes. Cycloadduct 30 obtained from (5S)-2 and cyclopentadiene was effectively elaborated to (1S,4S, 5R)-4-benzyloxycarbonylamino-2-oxabicyclo[3.3.0]oct-7-en-3-one (28), the key synthetic intermediate of carbocyclic polyoxin C.     

Synthesis and configuration of the nonadecenetriol isolated from seeds of Persea americana

In an effort to establish the relative as well as absolute configuration of the trypanocidally active natural nonadec-6-en-1,2,4-triol isolated from Persea americana, the (2S,4R), (2S,4S), and (2R,4R) isomers were synthesized. The stereogenic centers taken from enantiopure chiral epoxy building blocks derived from inexpensive and readily available D-glucolactone. The (2R,4R) isomer gave (1)H and (13)C NMR as well as specific rotation in excellent consistence with those reported for the natural triol.     

2-O-(2-hydroxybutyl)-beta-cyclodextrin as a chiral selector for the capillary electrophoretic separation of chiral drugs.

A new beta-cyclodextrin (beta-CD) derivative, 2-O-(2-hydroxybutyl)-beta-CD (HB-beta-CD), was successfully synthesized and used as chiral selector in capillary zone electrophoresis. Six chiral drugs, such as anisodamine, ketoconazole, propranolol, promethazine, adrenaline and chlorphenamine enantiomers, belonging to different classes of compounds of pharmaceutical interest were resolved. The chiral resolution (R(S)) was strongly influenced by the concentrations of the cyclodextrin derivative, the background electrolyte, and the pH of the background electrolyte. Under the conditions of 50 mmol/L tris-phosphate buffer at pH 2.5 containing 5 mmol/L 2-O-(2-hydroxybutyl)-beta-CD, the baseline separation of enantiomers, such as anisodamine (R(S) = 3.10), ketoconazole (R(S) = 3.01), propranolol (R(S) = 3.87), promethazine (R(S) = 3.63), adrenaline (R(S) = 3.42) and chlorphenamine (R(S) = 2.96), could be achieved.     

A concise synthesis of topsentin A and nortopsentins B and D

[reaction: see text] A concise synthesis of topsentin A (R(1) = R(2) = H) and nortopsentins B (R(1) = Br, R(2) = H) and D (R(1) = R(2) = H) is described from oxotryptamine 5 via reduction of acyl cyanide 4. Regiospecific bromination of 3-cyanoindole afforded 6-bromo-3-cyanoindole (10) as the major product.     

单组分酚膦中性镍催化乙烯均聚与共聚反应

以酚膦化合物为双齿配体,合成与表征了一系列单组分中性镍烯烃聚合催化剂。 研究表明,酚膦配体结构显著影响中性镍的催化性能,酚氧邻位无取代基的(2-PPh2-C6H4O)Ni(Me)(Py)(3a)活性较低,向酚氧邻位引入叔丁基或苯基等位阻基团可大幅度提高(2-PPh2-C6H3(R)O)Ni(Me)(Py)(3b~3d)的催化效率,最高催化活性可达4.46×106 g PE/(mol(Ni)·h)。 同时,聚乙烯的分子量也可以通过取代基效应进行适度调控,使用酚氧邻位带有苯基或蒽基的催化剂(3c~3d)可获得较高分子量的聚乙烯。 用供电子叔丁基替代二苯膦的一个苯环可提高催化活性中心镍原子的电子云密度,使辅助配体吡啶更容易离去,从而可在较低温度下引发乙烯聚合反应。 此外,这类酚膦中性镍催化剂对极性基团具有较强的耐受性,可催化乙烯与极性5-降冰片烯-2-乙酸酯的共聚反应。     

Iron complexes for the catalytic transfer hydrogenation of acetophenone: steric and electronic effects imposed by alkyl substituents at phosphorus

A series of iron(II) complexes, trans-[Fe(NCMe)(2)(PR(2)CH(2)CH═NCH(2)CH(2)N═CHCH(2)PR(2))][BPh(4)](2) (5, R = Cy; 7, R = iPr; 9, R = Et) were prepared via the template synthesis in one-pot involving air-stable phosphonium dimers, [cyclo-(-PR(2)CH(2)CH(OH)-)(2)](Br)(2) (4, R = Cy; 6, R = iPr; 8, R = Et), KOtBu, [Fe(H(2)O)(6)][BF(4)](2) and ethylenediamine in acetonitrile. In the synthesis of 9, a methanol/acetonitrile solvent mixture was required; otherwise an intermediate iron bis(tridentate) complex, [Fe(PEt(2)CH(2)CH═NCH(2)CH(2)NH(2))(2)](2+), formed as determined by electrospray ionization mass spectrometry (ESI-MS). The crude iron(II) complexes from a template synthesis with ethylenediamine or (S,S)-1,2-diphenylethylenediamine are stirred in acetone under a CO atmosphere (～2 atm) overnight to displace a NCMe ligand; however, in addition to this, bromide displaces an NCMe ligand as well to form a new class of the iron complexes trans-[Fe(CO)(Br)(PR(2)CH(2)CH═NCHR'CHR'N═CHCH(2)PR(2))](+) (10 R = Cy, R' = H; (S,S)-11, R = Cy, R' = Ph; 12, R = iPr, R' = H; (S,S)-13, R = iPr, R' = Ph; 14, R = Et, R' = H; (S,S)-15, R = Et, R' = Ph). These complexes were isolated in moderate yields (55-84%) as tetraphenylborate salts. Complexes 10-15 were tested for the catalytic transfer hydrogenation of acetophenone in basic iso-propanol at 25 and 50 °C. The complexes 10-13 (where R = Cy or iPr) were inactive while the complexes 14 and (S,S)-15 (where R = Et) were active at 25 °C but had better activity at 50 °C. Complex (S,S)-15 was higher in activity than complex 14, achieving turnover frequencies as high as 4100 h(-1), conversions of acetophenone to (R)-1-phenylethanol as high as 80% and an enantiomeric excess (e.e.) of 50% in the product. As catalysis progressed, the e.e. diminished to as low as 26%.     

Substituent effects of beta-diketiminate ligands on the structure and physicochemical properties of copper(II) complexes

Substituent effects of beta-diketiminate ligands on the structure and physicochemical properties of the copper(II) complexes have been systematically investigated by using 3-iminopropenylamine derivatives R1LR3H, R3-N=CH-C(R1)=CH-NH-R3, where R1 is Me, H, CN, or NO2, and R3 is Ph, Mes (mesityl), Dep (2,6-diethylphenyl), Dipp (2,6-diisopropylphenyl), or Dtbp (3,5-di-tert-butylphenyl). When the ligands with R3=Ph or Dtbp were treated with CuII(OAc)2, bis(beta-diketiminate) copper(II) complexes exhibiting distorted tetrahedral geometries were obtained, the crystal structures of which were nearly the same as each other regardless of the alpha-substituent (R1); dihedral angles between the two beta-diketiminate coordination planes are 62.5 +/- 1.2 degrees, and the Cu-N bond lengths are 1.959 +/- 0.008 A. The distorted tetrahedral structures are maintained in solution, but the spectroscopic features, especially gII values of the ESR spectra and the d-d bands of the absorption spectra, as well as the electrochemical behaviors of the complexes, are significantly affected by the electronic nature of R1. The ligands with R3=Mes and Dep, on the other hand, gave di(mu-hydroxo)dicopper(II) complexes, and their crystal structures as well as spectroscopic and electrochemical features have also been explored. Furthermore, the ligand with the more sterically encumbered aromatic substituent (Dipp) provided a mononuclear four-coordinate square planar copper(II) complex supported by one beta-diketiminate ligand and one didentate acetate ion. Thus, the beta-diketiminate ligands with a variety of substituents (R1 and R3) have been explored to provide coordinatively unsaturated (four-coordinate) mononuclear and dinuclear copper(II) complexes with significantly different coordination geometry and properties.     

三苯甲基取代烯烃的环氧化研究

合成了6种三苯甲基取代烯烃. 以二甲基二氧杂环丙烷作为主要氧化剂, 在催化剂(R,R)-Salen Mn(III)的催化下, 进行不对称环氧化, 其不对称环氧化产物ee值较高(81%). 初步研究表明, 二甲基二氧杂环丙烷(DMD)和(R,R)-Salen Mn(III)的环氧化体系对于含亚甲基的三苯甲基取代的烯烃的氧化产率高但对映选择性差, 对于不含亚甲基的三苯甲基取代的烯烃的氧化产率低但对映选择性好.     

Liquid Chromatographic Resolution of Enantiomeric Dipeptides on the Chiral Stationary Phase Derived from (S)-1-(6,7-Dimethyl-1-naphthyl)isobutylamine

Abstract

Liquid chromatographic resolution of fifteen enantiomeric dipeptide methyl esters as their N-3,5-dinitrobenzoyl derivatives was investigated on the chiral stationary phase (CSP) derived from (S)-1-(6,7-dimethyl-1-naphthyl)isobutylamine. The four stereoisomers present in each dipeptide derivative were observed to be separated quite well with the (R,R) isomer being eluted first. The separation factors for two enantiomeric pairs such as (R,R)/(S,S) and (R,S)/(S,R) and the elution orders are explained by two competing “opposite-sense” chiral recognition mechanisms.     

Syntheses in enantiopure form of four diastereoisomeric naphthopyranquinones derived from aphid insect pigments

The first syntheses are described of the four enantiopure naphthopyranquinones (1R,3R,4S)- and (1R,3R,4R)-3,4-dihydro-4,7,9-trihydroxy-1,3-dimethylnaphtho[2,3-c]pyranquinone (quinone A 1 and quinone A' 2) and their two C-3 epimers, the (1R,3S,4S)- and (1R,3S,4R)-diastereoisomers 5 and 6, using enantiopure lactate as the source of asymmetry. Key factors in these syntheses are the maintenance of stereochemical integrity throughout the sequences and intramolecular diastereoselective cyclisations of the titanium phenolates of phenolic lactaldehydes. For these cyclisations the differing degree of diastereoselectivity is explained as are the stereochemistries of the product 2-benzopyran-4,5-diols.     

Preparation of propargyl hydroperoxides by regioselective oxidation of allenic zinc reagents with molecular oxygen

Treatment of allenic zinc reagents (R(1)R(2)C[double bond]C[double bond]C(R(3))ZnL), generated by the reaction of propargyl derivative (R(1)R(2)C(X)[triple bond](CH) with triorganozincates (R(3)(3)ZnLi), under oxygen atmosphere in the presence of ZnCl(2) and chlorotrimethylsilane afforded propargyl hydroperoxides (R(1)R(2)C(OOH)C[triple bond];CR(3)) regioselectively. In this reaction, the use of ZnCl(2) and chlorotrimethylsilane as additives is essential for the transformation of the initially generated allenic reagents to more reactive chlorozinc species.