Resolution of α-phenylethylamine by its acidic derivatives

α-Phenylethylamine was resolved by its own derivatives formed with a homologous series of dicarboxylic acids. The structure of the oxalamic acid diastereoisomeric salts was investigated by the single-crystal X-ray diffraction method.     

Cyclization of α-furylmethyl derivatives of linalool by "activated" DMSO

The cyclization of two stereoisomeric -furylmethyl derivatives of linalool initiated by "activated" DMSO leads to the corresponding substituted limonene in low yield. The stereochemistry of these products was not established.N. D. Zelinskii Institute of Organic Chemistry, Russian Academy of Sciences, 117913 Moscow, B-334. Translated from Izvestiya Akademii Nauk, Seriya Khimicheskaya, No. 2, pp. 471–473, February, 1992.     

Reaction Routes of Free Radicals in γ-Irradiated α-D-Glucose

-Irradiated -D-glucose was studied over a wide temperature range (77–415 K) using ESR and product analysis techniques. A plausible scheme of the radiation-induced degradation of -D-glucose is proposed.     

Stereoselective synthesis of tetrahydropyran new derivatives underlain by α-allyl ketones

Decarboxylation of α-allyl-substituted acetoacetic esters afforded α-allyl ketones that were reduced with L-selectride [LiBH(s-Bu)₃] in alcohols RCH(OH)CH₂CH₂CH=C(Me)CH₂R'. The latter reacted with methyl 4-hydroxy-3-formylbenzoate and methyl orthoformate in the presence of p-toluenesulfonic acid to provide trans-tetrahydropyrano[3,2-с][1]benzopyran. In reaction of the E-isomer of alcohol Me₂CHCH(OH) CH₂CH₂CH=C(Me)CH₂CH₂Ph with CF₃SO₃H a stereoselective cyclization occurred with the formation of 2,6-disubstituted tetrahydropyran; Prins reaction with 4-bromobenzaldehyde and salicylaldehyde in the presence of boron trifluoride etherate also proceeded stereoselectively giving a substituted tetrahydropyrano-[3,2-c][1]-benzopyran.     

Oxidation of the α-ketol and enone derivatives of cyclohexanone by tetrazolium salts

A new red-ox reaction, leading to the respective keto derivatives from α-ketol and enone derivatives of cyclohexanone, is reported.     

Enantioselective α-hydroxylation of β-keto esters catalyzed by chiral S-timolol derivatives

A screen of aryloxy aminopropanol organocatalysts derived from the β-blocker inhibitor S-timolol determined the most active catalyst of asymmetric α-hydroxylation of β-keto esters. (R)-1-(tert-butylamino)-3-(3,4,5-trimethoxyphenoxy) propan-2-ol (3k) was the most effective derivative, enantioselectively catalyzing α-hydroxylation of β-keto esters using tert-butyl hydroperoxide as the oxidant in hexane to afford the corresponding products in excellent yield and with good enantioselectivity (up to 96% yield, 88% ee).     

Catalytic stereoselective synthesis of α-Amino phosphonic acid derivatives by asymmetric hydrogenation

The phosphonate analogue of α-N-benzoyl protected phenylalanine methylester has been prepared by catalytic synthesis. Commonly used Rh-complexes has been applied in asymmetric hydrogenation to check their usefulness in the standard reaction.     

Synthesis of trialkylaluminum derivatives by the reaction of non-solvated aluminum hydride with α-olefins

Hydroalumination of -olefins by non-solvated polymeric aluminum hydride (AlH₃) _n occurs at 120—140 °C. Mechanochemical activation accelerates this reaction. The addition of catalytic amounts of the prepared R₃Al forms to the reaction system decreases the temperature of the process to 90—100 °C. The greatest initiation effect is observed when ate-complexes of the MAlR₄ type (M = Li, Na) are used: the reaction occurs with a higher rate already at 60—90 °C affording R₃Al free of admixtures of carbalumination products and dimers of -olefins.     

Conformational investigation of α-methylthio and α-phenylthio derivatives of acetone and cyclohexanone by molecular mechanics. An x-ray study of α-phenylthioacetone

A conformational investigation of -methylthioacetone, -methylthiocyclohexanone, -phenylthioacetone, and -phenylthiocyclohexanone was undertaken in the MM2(87) force field. In all cases theac-G rotamers with unidirectional orientation of the C=O and S-R bonds are preferred in accordance with the experimental investigations. In all cases the energy of dipole-dipole interaction makes a contribution to the stabilization of these forms. For the eclipsedsp conformers the relatively high calculated values of the energies contradict the data of the experimental investigations, which take account of their participation in the equilibrium. X-ray crystallographic analysis of -phenylthioacetone (3) showed that thesp-T structure with a planar orientation of the thioanisole fragment is realized in the solid phase.A. E. Arbuzov Institute of Organic and Physical Chemistry, Kazan' Scientific Center, Russian Academy of Sciences, 420083 Kazan'. Translated fromIzvestiya Akademii Nauk, Seriya Khimicheskaya, No. 6, pp. 1364–1371, June, 1992.     

Preparation of chiral α-diazophosphonic acid derivatives

The chiral α-diazophosphonic acid derivatives 3, 6 and 8 were prepared from (−)-ephedrine and (S,S)-N,N′-dimethyl-1,2-diaminocyclohexane; preliminary experiments suggest that the chiral auxiliary exerts little influence in the dirhodium(II) acetate catalysed OH and NH insertion reactions.     

Novel intramolecular photocyclization of α-arylthiophene derivatives

Photoirradiation of α-arylthiophene derivatives linked with an alkene moiety through a three-atom spacer gave unprecedented cyclobutene-fused perhydrothiapentalene-type compounds in high yields, but neither [2 + 2] nor [4 + 2] cycloaddition products. The reaction afforded a single diastereomer in many cases. The chemical structure and relative configuration of a typical product were unambiguously determined by X-ray crystallographic analysis.     

Synthesis of protected α-alkyl lanthionine derivatives

Protected α-alkyl lanthionine derivatives were synthesized in five steps starting from a known phenyloxazoline precursor. This approach involved the synthesis of a family of substituted cyclic sulfamidates and their regioselective opening by nucleophilic attack with a protected cysteine. This efficient multistep strategy affords various α-alkylated lanthionine derivatives in high yields.     

Synthesis of α-sulfanyl-β-amino acid derivatives by using nanocrystalline magnesium oxide

The Mannich-type reaction between alkyl, aryl and heterocyclic aldimines and sulfonium salts for the synthesis of α-sulfanyl-β-amino acid derivatives by using nanocrystalline magnesium oxide (NAP-MgO) is described. These products are obtained in moderate to high yields with moderate diastereoselectivities. The configuration of ethyl-3-{[(4-methylphenyl)sulfonyl]amino}-2-(methylsulfanyl)-3-(4-nitrophenyl)propanoate (major isomer) has been confirmed by X-ray diffraction technique to be anti, and consistent with the assignment based on ¹H NMR spectroscopy. These α-sulfanyl-β-amino acid derivatives are important building blocks for pharmaceuticals with potent biological activity.     

Enantioselective α-chlorination of β-oxo esters catalyzed by chiral diterpenoid alkaloid derivatives

Easily accessible diterpenoid alkaloid derivatives have been used as organocatalysts in the enantioselective α-chlorination of β-oxo esters. The treatment of β-oxo esters with N-chlorophthalimide (NCP) as a chlorine source under mild reaction conditions afforded the corresponding α-chlorinated β-oxo esters in excellent yields (up to 98%) and with moderate enantioselectivities (up to 68% ee) in 30 min.     

Inhibition of cyclodextrins on the activity of α-amylase

α-amylase activity influences both flour fermentation process and the quality of the fermented products due to its ability of breaking starch into smaller units. The inhibition of cyclodextrins on α-amylase activity was investigated in this paper. Experiment results showed that hydrophobic cavity size was an intrinsic factor during the inhibition processing. Among three types of cyclodextrin (α-, β- and γ-), β-type exhibited the most significant inhibitory activity toward α-amylase. The optimal inhibitory parameters were indicated to be pH 5.9, concentration of β-cyclodextrins 1 mmol/L, reaction temperature 45 °C and reaction time 60 min. Results suggested that the endogenous fluorescence of α-amylase was inhibited by cyclodextrins. Circular dichroism spectrum indicated that the secondary structure of α-amylase, including α-helices, β-sheets and random coils, was changed by cyclodextrins. All the results in this paper aim to provide a further understanding for α-amylase in the industry application.     

Complete Solid State 13C NMR Chemical Shift Assignments for α-D-Glucose, α-D-Glucose-H2O and β-D-Glucose

Abstract

NMR spectra of crystalline α-D-glucose DH₂O (1), α-D-glucose (2), and β-D-glucose (3) were examined by 13C cross polarization magic angle spinning (CPMAS) methods. Each of the three forms of glucose exhibited a distinctly different spectrum. Chemical interconversion of 2 and 3 as well as the in situ dehydration of 1 during the course of the CPMAS NMR experiment was monitored in the ¹³C spectra. Samples of 1, 2, and 3 specifically enriched at C-1 and C-6 with ¹³C yielded ¹³C spectra in which the resonances corresponding to the adjacent C-2 and C-5 carbons were not visible due to strong homonuclear ¹³C dipolar interactions with the high abundance label. Spectra of these analogues as well as the C-2 and C-3 labeled materials provided the complete ¹³C chemical shift assignments of crystalline 1 2, and 3. A comparison of the solid state and solution ¹³C spectra revealed substantial resonance shifts for each of the three structures examined.     

Synthesis of novel carboranyl derivatives of α-amino acids

New routes to closo-carboranyl derivatives of L-lysine and L-glutamic acid with free gA-NH2 groups were proposed.     

Inhibition mechanism of human salivary α-amylase by lipid transfer protein from Vigna unguiculata

VuLTP1.1, a LTP1 from Vigna unguiculata, inhibits 78.1 % of the human salivary α-amylase (HSA) activity at 20 μM. We had performed a correlation study between VuLTP1.1 structure and HSA inhibitory activity and showed that two VuLTP1.1 regions are responsible for HSA inhibition. In one of them we had characterized the crucial importance of an Arg₃₉ for inhibition. In this work, we analyzed the VuLTP1.1-HSA interaction by protein-protein docking to understand the most probable interaction model and the mechanism of HSA inhibition by VuLTP1.1. The VuLTP1.1 tertiary structure quality and refinement as well as the docking assay between VuLTP1.1 and HSA were done by bioinformatic programs. HSA inhibition occurs by direct interaction of the VuLTP1.1 with the HSA causing the obstruction of the carbohydrate biding cleft with Gibbs free energy of -18.5 Kcal/mol and the dissociation constant of 2.6E⁻¹⁴ M. The previously identified Arg₃₉ of VuLTP1.1 is burrowed into the active site of the HSA and there it interacts with the Asp₃₀₀ of HSA catalytic site by a hydrogen bond. We had confirmed the importance of the Arg₃₉ of VuLTP1.1 for the HSA inhibition which interacts with the Asp₃₀₀ at the HSA active site. I-2, a LTP-like peptide, presents the same HSA inhibition pattern that VuLTP1.1, which indicates that the inhibition mechanism of the LTPs towards α-amylase is very similar. For the best of our knowledge, it is the first time that the HSA inhibition mechanism was understood and described for the LTP1s using VuLTP1.1 and I-2 as prototype inhibitors.