Enzymatic Enantioselective Synthesis of （R）－2－Trimethylsilyl－2－hydroxyl－propionitrile by Defatted Apple Seed Meal

IntroductionOverthepastyears ,thesynthesisofchiralaldehyde cyanohydrinswaswellstudied .1Incontrasttochiralalde hyde cyanohydrins ,therewereonlyfewreportsaboutthepreparationofopticallyactiveketone cyanohydrins ,2 whichareusefulstartingmaterialsandintermediatesforthesyn thesisofmanychiralnaturalproducts .3Wethereforefo cusedonthepreparationofopticallyactivesiliconcontain ing (R ) ketone cyanohydrin ((R ) 2 trimethylsilyl 2 hy droxyl propionitrile)usingacetonecyanohydrinastran scyanationagen…     

具有C2对称的氮磷-氧磷配体双噁唑啉磷乙烷的合成及在不对称催化加氢中的应用

利用易得的光学纯N-甲基氨基醇与1,2-双(二氯磷)乙烷缩合合成了一类新的具有C₂对称轴的氮磷-氧磷配体(R,R)-双噁唑啉磷乙烷(BOAPE) 1～4. 该类配体不仅具有C₂对称结构和刚性五元环, 还具有富电子特性, 利用500 MHz进行了¹H NMR, ³¹P NMR, ¹³C NMR表征. 与这些配体配位形成的Rh配合物用于N-苯甲酰基脱氢丙氨酸衍生物和α-功能化酮不对称加氢, 分别可以得到99%和98%的ee. 这类配体比它们相对应的非C₂对称的氮磷-氧磷化合物(AMPP)配体具有更高的对映选择性. 在这四个新的配体中配体(R,R)-Ph-BOAPE (2)的催化性能最优. 催化剂[Rh(COD)(R,R)-Ph-BOAPE]BF₄的半反应周期t_1/2和周转频率(TOF)在N-苯甲酰基肉桂酸甲酯的不对称加氢反应中分别为12 min和6.5 min^－1.     

O,O'-Di-p-toluoyl-(2R,3R)-tartaric acid as supramolecular resolving agent

O,O'-di-p-toluoyl-(2R,3R)-tartaric acid (DPTTA) was investigated as supramolecular complex (SMC) forming resolving agent with three racemic alcohols (menthol, 4-methyl-2-pentanol, trans-2-iodo-cyclohexanol) by preparative scale experiments and thermoanalytical measurements. Despite the very small structural difference (two methyl groups) between the O,O'-dibenzoyl-(2R,3R)-tartaric acid (DBTA) and DPTTA, their SMC forming properties with water and racemic alcohols is very different. While DBTA forms SMC with all the three investigated alcohols, DPTTA forms SMC only with trans-2-iodo-cyclohexanol. DPTTA binds the guest compound less strongly and the stoichiometry of the SMC is also different. The weaker interactions resulted in less effective optical resolutions. The results of these investigations remind us, that in optical resolutions during the chiral discrimination process the weaker interactions have a determining role, since DBTA and DPTTA have the possibility to form the same strong (O-H···O and N-H···O) hydrogen bond network. This revised version was published online in August 2006 with corrections to the Cover Date.     

Synthesis,characterization, and organocatalytic application of chiral ionic liquids derived from (S,R)-noscapine

(S,R)-Noscapine, a phthalideisoquinoline alkaloid has been used as precursor for the synthesis of chiral ionic liquids (CILs). Noscapine based CILs have been synthesized from reaction between (S,R)-noscapine and methyl iodide in acetonitrile at room temperature. The synthesized CILs have been characterized by ¹H NMR, ¹³C NMR, EI-MS, and polarimetry techniques. These CILs have been used as organocatalysts in the enantioselective reduction of prochiral ketones to produce optically active secondary alcohols. The optically active secondary alcohols have been obtained with excellent yields and low to moderate enantiomeric excess (ee); also the complete enantiomeric excess (100% ee) has been achieved in some cases.     

Microbial carbonylation and hydroxylation of 20(R)-panaxadiol by Aspergillus niger

20(R)-panaxadiol (PD) was metabolised by the fungus Aspergillus niger AS 3.3926 to its C-3 carbonylated metabolite and five other hydroxylated metabolites (1–6). Their structures were elucidated as 3-oxo-20(R)-panaxadiol (1), 3-oxo-7β-hydroxyl- 20(R)-panaxadiol (2), 3-oxo-7β,23α-dihydroxyl-20(R)-panaxadiol (3), 3,12-dioxo- 7β,23β-dihydroxyl-20(R)-panaxadiol (4), 3-oxo-1α,7β-dihydroxyl-20(R)-panaxadiol (5) and 3-oxo-7β,15β-dihydroxyl-20(R)-panaxadiol (6) by spectroscopic analysis. Among them, compounds 2–6 were new compounds. Pharmacological studies revealed that compound 6 exhibited significant anti-hepatic fibrosis activity.     

Synthesis of cannabinoid model compounds. Part 2: (3R, 4R)-Δ1(6)-Tetrahydrocannabinol-5″-oic acid and 4″(R,S)-Methyl-(3R, 4R)-Δ1(6)-tetrahydrocannabinol-5″-oic Acid

Two novel cannabinoid model compounds, (3R, 4R)-Δ¹⁽⁶⁾-tetrahydrocannabinol-5″-oic acid (22) and 4″(R, S)-methyl-(3R, 4R)-Δ¹⁽⁶⁾-tetrahydrocannabinol-5″-oic acid (23) were synthesized by acid-catalyzed condensation of (+)-trans-p-mentha-2, 8-dien-l-ol (1) with the substituted resorcinols 18 and 19 obtained by a Wittig reaction between 3, 5-bis(benzyloxy)benzaldehyde (7) and methyl 4-bromobutanoate (10) or methyl 4-bromo-2(R, S)-methylbutanoate (11) resp. with subsequent hydrogenation. The resulting methyl esters 20 and 21 were hydrolyzed to give acids 22 and 23 .     

Synthesis of (5R,8S,10R)-6-(Allyloxy)- and (5R,8S,10R)-6-(Propyloxy)ergolines from the 6-Methyl Precursors

Novel (5R,8S,10R)-6-(allyloxy)- and (5R,8S,10R)-6-(propyloxy)ergolines have been synthesized by use of a Meisenheimer [2,3]-sigmatropic rearrangement of a (5R,8S,10R)-6-allyl-ergoline N⁶-oxide as key step.     

利用工业废弃物中获得的(R)-5-甲基-δ-戊酸内酯为原料合成(2R,6R)-2,6,10-三甲基十一醇

(2R,6R)-2,6,10-三甲基十一醇(1)是维生素E、维生素K和植醇的基本结构单元. 利用从甾体皂甙元氧化降解产生的工业废弃物中所获得的手性化合物(R)-5-甲基-δ-戊酸内酯(6), 先将其转化成为化学性质稳定的(4R)-甲基-5-甲氧甲氧基戊酸甲酯(7), 再经十二步反应, 以14.1%的总收率合成得到了目标化合物(2R,6R)-2,6,10-三甲基十一醇(1).     

Synthesis of New Chiral Calix [4] crown Containing (R)‐Cysteine

Three new chiral heterocalix [4] crowns containing aza thio atoms bearing two chiral sites provided by (R)‐cysteine ester were synthesized. All new compounds were characterized by ¹H NMR, MS and elemental analysis.     

A Facile Synthesis of Enantiomerically Pure (R)‐6‐Arylbinols

This work reported a convenient method for the preparation of enantiomerically pure 6‐aryl‐2,2′‐dihydroxy‐1,1′‐binaphthyl derivatives starting from the commercially available (R)‐2,2′‐hydroxy‐1,1′‐binaphthyl [(R)‐ 1 ] via bromination, hydrolysis and Suzuki cross coupling reaction. This novel synthetic method was characterized with high regioselectivity, simple operation, mild reaction conditions, and excellent yield (up to 73%). On the other hand, we synthesized the target unknown compounds, which were confirmed by IR, ¹H NMR, ¹³C NMR, MS and elementary analysis.     

Über den Phosphandiyl‐Transfer von invers‐polarisierten Phosphaalkenen R1P=C(NMe2)2 (R1 = tBu,Cy, Ph,H) auf Phospheniumkomplexe [(η5‐C5H5)(CO)2M=P(R2)R3] (R2 = R3 = Ph; R2 = tBu,R3 = H; R2 = Ph,R3 = N(SiMe3)2)

Phosphanediyl Transfer from Inversely Polarized Phosphaalkenes R¹P=C(NMe₂)₂ (R¹ = tBu, Cy, Ph, H) onto Phosphenium Complexes [(η⁵‐C₅H₅)(CO)₂M=P(R²)R³] (R² = R³ = Ph; R² = tBu, R³ = H; R² = Ph, R³ = N(SiMe₃)₂) Reaction of the freshly prepared phosphenium tungsten complex [(η⁵‐C₅H₅)(CO)₂W=PPh₂] ( 3 ) with the inversely polarized phosphaalkenes RP=C(NMe₂)₂ ( 1 ) ( a : R = tBu; b : Cy; c : Ph) led to the η²‐diphosphanyl complexes ( 9a‐c ) which were isolated by column chromatography as yellow crystals in 24‐30 % yield. Similarly, phosphenium complexes [(η⁵‐C₅H₅)(CO)₂M=P(H)tBu] (M = W ( 6 ); Mo ( 8 )) were converted into (M = W ( 11 ); Mo ( 12 )) by the formal abstraction of the phosphanediyl [PtBu] from 1a . Treatment of [(η⁵‐C₅H₅)(CO)₂W=P(Ph)N(SiMe₃)₂] ( 4 ) with HP=C(NMe₂)₂ ( 1d ) gave rise to the formation of yellow crystalline ( 10 ). The products were characterized by elemental analyses and spectra (IR, ¹H, ¹³C‐, ³¹P‐NMR, MS). The molecular structure of compound 10 was elucidated by an X‐ray diffraction analysis.     

Ternary Rare Earth Metal Palladium and Platinum Aluminides R4Pd9Al24 and R4Pt9Al24

The fifteen intermetallic compounds R₄Pd₉Al₂₄ (R = Gd–Tm) and R₄Pt₉Al₂₄ (R = Y, Gd–Lu) were prepared by reaction of the elemental components. Their crystal structure was determined from single-crystal X-ray data of Er₄Pt₉Al₂₄. It is pseudo-trigonal with triclinic symmetry: P 1, a = b = 747.5(2) pm, c = 1306.7(4) pm, α = 100.99(2)°, β = 95.47(2)°, γ = 60.00(3)°, Z = 1, R = 0.052 for 2593 structure factors and 110 variable parameters. The structure is closely related to that of Y₂Co₃Ga₉. Both may be described as stacking variants of each other. They consist of layers of the compositions PtAl₂ (CoGa₂), and Er₂Al₃ (Y₂Ga₃), designated A and B, respectively. These layers are stacked in the five- and four-layer sequences ABAAB (Er₄Pt₉Al₂₄) and ABAB (Y₂Co₃Ga₉). The layers PtAl₂ and CoGa₂ are similar to the hexagonal close packed layers in the TiSi₂-, CrSi₂-, and MoSi₂-type structures. The structure of Er₄Pt₉Al₂₄ contains a monoclinic subcell, where the layers Er₂Al₃ are disordered. A partial disorder of this kind, which could be ascribed to twinning or to the intergrowth with another stacking variant, was found during the structure refinement of the isotypic compound Y₄Pt₉Al₂₄: a = b = 749.0(2) pm. c = 1309.3(4) pm, α = 100.99(2)°, β = 95.48(2)°, γ = 60.00(3)°, R = 0.031 for 1435 structure factors and 128 variable parameters.     

Tolterodinium (+)‐(2R,3R)‐hydrogen tartrate

In the crystal structure of (R)‐N,N‐diisopropyl‐3‐(2‐hydroxy‐5‐methyl­phenyl)‐3‐phenyl­propyl­aminium (2R,3R)‐hydrogen tartrate, C₂₂H₃₂NO⁺·C₄H₅O₆⁻, the hydrogen tartrate anions are linked by O—H⋯O hydrogen bonds to form helical chains built from (9) rings. These chains are linked by the tolterodine molecules via N—H⋯O and O—H⋯O hydrogen bonds to form separate sheets parallel to the (101) plane.     

Asymmetric oxidation of sulfides catalyzed by (R)-6,6'-dibromo-BINOL derived titanium complex

Abstract

An efficient asymmetric oxidation of sulfides was achieved using (R)-6,6'-dibromo-BINOL as chiral ligand in combination with Ti(OⁱPr)₄ using 70% aqueous tertiary butyl hydroperoxide as oxidant. The resulting sulfoxides had high enantiopurities and good yields. A range of aryl alkyl and aryl benzyl sulfides were oxidized to the corresponding sulfoxides with 78–95% ee in 72–80% yields.     

Synthesis of (+)-1,3:2,5-dianhydroviburnitol ((+)-(1R,2R,3S,5R,6S)-4,7-dioxatricyclo[3.2.1.03,6]octan-2-ol)

Epoxidation of (?)-(1R,2R,4R)-2-endo-cyano-7-oxabicyclo[2.2.1]hept-5-en-2-exo-yl acetate ((?)-5) followed by saponification afforded (+)-(1R,4R,5R,6R)-5,6-exo-epoxy-7-oxabicyclo[2.2.1]heptan-2-one ((+)-7). Reduction of (+)-7 with diisobutylaluminium hydride (DIBAH) gave (+)-1,3:2,5-dianhydroviburnitol ( = (+)-(1R,2R,3S,4R,6S)-4,7-dioxatricyclo[3.2.1.0^3,6]octan-2-ol; (+)-3). Hydride reductions of (±)-7 were less exo-face selective than reductions of bicyclo[2.2.1]heptan-2-one and its derivatives with NaBH₄, AlH₃, and LiAlH₄ probably because of smaller steric hindrance to endo-face hydride attack when C(5) and C(6) of the bicyclo-[2.2.1]heptan-2-one are part of an exo oxirane ring.     

Calorimetric and theoretical studies on the system of {(R)-(+)-limonene+(S)-(-)-limonene}

In order to reveal the origin of chiral discrimination, excess molar heat capacities (C_P ^E) of ((R)-(+)-limonene+(S)-(−)-limonene) were determined by using a differential scanning calorimeter at temperatures between T=293.15 and 303.15 K. All C_P ^E curves show S-shape. It was inferred that randomness appears in the (S)-(-)-limonene-rich region, and that non-randomness appears in the (R)-(+)-limonene-rich region. To clarify the differences in homochiral interactions and heterochiral interactions, molecular orbital calculations were carried out.     

Microbial transformation of cannabinoids. Part 3: Major metabolites of (3R, 4R)-Δ1-tetrahydrocannabinol

The metabolic transformations of the psychotropic cannabinoid (3R, 4R)-Δ¹-tetrahydrocannabinol (5) (=Δ¹-THC) by cultures of Fusarium Nivale, Gibberella fujikuroi (both Ascomycetes) and Thamnidium elegans (Phycomycetes) were investigated. A number of metaboilites, 1–4 and 6–9 were isolated from the incubations, partly purified and their structures elucidated by combined gas chromatography/mass spectrometry. Four of these metabolites, 1″-hydroxy-Δ¹-THC (4) 2″-hydroxy-β¹-THC (1) 6Δ-hydroxy-ζ¹-THC (8) and 2″,6Δ-dihydroxy-Δ¹-THC (9) so far have not been reported as microbial transformation products of 5 .     

Chiral Separation of (R,R)-Tadalafil and Its Enantiomer in Bulk Drug Samples and Pharmaceutical Dosage Forms by Chiral RP-LC

A new simple isocratic chiral RP-LC method has been developed for the separation and quantification of the enantiomer of (R,R)-tadalafil in bulk drugs and dosage forms with an elution time of about 20 min. Chromatographic separation of (R,R)-tadalafil and its enantiomer was achieved on a bonded macro cyclic glycopeptide stationary phase. The method resolves the (R,R)-tadalafil and its enantiomer with a resolution (R _s) greater than 2.4 in the developed chiral RP-LC. The mobile phase used for the separation and quantification of (R,R)-tadalafil and its enantiomer involves a simple mixture of reverse phase solvents and the cost of analysis was drastically decreased. The test concentration is 0.4 mg mL⁻¹ in the mobile phase. This method is capable of detecting the enantiomer of (R,R)-tadalafil up to 0.0048 μg wrt test concentration 400 μg mL⁻¹ for a 20 μL injection volume. The drug was subjected to stress conditions of hydrolysis, oxidation, photolysis and thermal degradation. There was no interference of degradants with (R,R)-tadalafil and its enantiomer in the developed method. The developed chiral RP-LC method was validated with respect to linearity, accuracy, precision and robustness. The percentage recovery for the enantiomer of (R,R)-tadalafil in bulk drug samples and in dosage forms ranged from 97.0 to 102.5%. The test solution was found to be stable in the mobile phase for 48 h after preparation.     

HRGC separation of hydroperoxides formed during the photosensitized oxidation of (R)—(+)-Limonene

(R)—(+)-Limonene was photooxidized in the presence of Rose Bengal as catalyst. After TLC isolation, the hydroperoxides formed were separated directly by HRGC and analyzed by MS (El; Cl). Each hydroperoxide isomer was then isolated by HPLC for structure determination which after reduction of the HOO group with sodium borohydride was performed by ¹H-NMR and ¹³C-NMR. Six hydroperoxide isomers formed by oxidation of the endocyclic double bond were identified. The compounds eluted from the HRGC column in the following order (proportions are given in brackets) I (40.1%) (1S, 4R)-p-mentha-2, 8-diene 1-hydroperoxide; II (5.8%) (1R, 4R)-p-mentha-2, 8-diene 1-hydroperoxide; III (20.6%) (2R, 4R)-p-mentha-[1(7), 8]-diene 2-hydroperoxide; IV (8.5%) (2R, 4R)-p-mentha-6, 8-diene 2-hydroperoxide; V (4%) (2S, 4R)-p-mentha-6, 8-diene 2-hydroperoxide; and VI (21.0%) (2S, 4R)-p-mentha-[1(7), 8]-diene 2-hydroperoxide. Direct HRGC separation of the limonene hydroperoxides offers, inter alia, the possibility of determining their flavor qualities by HRGC/effluent sniffing.     

(5R*, 9S*)- and (5R*, 9R*)-2,2,9-Trimethyl-1,6-dioxaspiro[4.4]non-3-ene and their Dihydro Derivatives as New Constituents of Geranium Oil

(5 R^*,9S^*)- and (5R^*,9R^*)-2,2,9-Trimethyl-1,6-dioxaspiro [4.4]non-3-ene ( 1a and 1b resp.) and their dihydro derivatives 2a and 2b are described as new constituents of geranium oil. The structures and configurations of 1a , 1b , 2a , and 2b , are based on spectra interpretation and syntheses. Also some other monoterpenoid constituents identified in the same boiling range are discussed.