Synthesis of ribonucleoside analogues containing thio-substituted 1,3,4-triazole as heterocyclic base

New ribonucleoside analogues containing thio-substituted 1,3,4-triazole as heterocyclic base have been synthesized via condensation of the central intermediate 1 with various acids,esters,amides,and anhydrides in anhydrous solvent followed by deprotection.     

Synthesis and bioactivity of α-galactosylceramide analogues bearing an aryl group within the fatty amide chain

We describe the synthesis and bioactivity of analogues of α-galactosylceramide (1) bearing a long-chain alkyl group substituted at the meta or para position of an aryl group embedded within the amide chain. We compared the ability of these compounds and of 1 and C6Ph (2, which has a phenyl group at the amide chain terminus) to stimulate murine invariant Natural Killer T cells and to dock with human CD1d.     

Synthesis of optically active α-bromohydrins via reduction of α-bromoacetophenone analogues catalyzed by an isolated carbonyl reductase

Enantiomerically pure (S)-α-bromohydrins were prepared by the reduction of α-bromoacetophenone analogues catalyzed by an isolated carbonyl reductase from Candida magnolia with high yield and excellent enantiomeric excess when methyl tert-butyl ether was employed as the co-solvent, while avoiding the formation of by-products. This provides a new approach to access these chiral α-bromohydrins which are of pharmaceutical importance.     

Synthesis of an Acyloxymethyl Prodrug of the Inositol Phosphate α-Trinositol

ABSTRACT

Acyloxymethylation of an acylated silver salt of α-trinositol gives, after deprotection, membrane permeable 1D-myo-inositol 1,2,6-tris(ethoxycarbonyloxymethyl sodium phosphate). The acyl groups, 3-(4,5-methylenedioxy-2-nitrophenyl)propanoyl, are cleaved by hydrogenolysis.     

Novel galactosyl donor with 2-naphthylmethyl (NAP) as the non-participating group at C-2 position: efficient synthesis of α-galactosyl ceramide

Predominant α-linked products can be generated in glycosylation involving galactosyl trichloroacetimidate donors with 2-naphthylmethyl (NAP) as the non-participating group at C-2 position. The above-mentioned donor was successfully utilized for the synthesis of α-galactosyl ceramide.     

Synthesis of arylglycine and mandelic acid derivatives through carboxylations of α-amido and α-acetoxy stannanes with carbon dioxide

Incorporation reactions of carbon dioxide (CO(2)) with N-Boc-α-amido and α-acetoxy stannanes were developed using CsF as a mild tin activator. Monoprotected α-amido stannanes could be used, and the corresponding arylglycine derivatives were obtained in moderate-to-high yields under 1 MPa (10 atm) of CO(2) pressure. α-Acetoxy stannanes also underwent carboxylation to afford mandelic acid derivatives in excellent yields under ambient CO(2) pressure. Both transformations enabled the synthesis of α-tertiary and α-quaternary carboxylic acid derivatives. In addition, the chirality of (S)-N-tert-butylsulfonyl-α-amido stannanes was transferred with up to 90% inversion of configuration at 100 °C.     

Chiral Synthesis of an α-Tetrasubstituted Proline Derivative

An efficient approach for the synthesis of a new class of triazolophanes by 1,3-dipolar cycloaddition reaction of highly reactive organic azides with dialkynes using Cu(I)-catalyzed azide–alkyne cycloaddition methodology (“click chemistry”) has been developed. All the compounds were characterized by spectral and elemental analyses.     

Synthesis of RGD analogues containing α-Tfm-arginine as potential fibrinogen receptor antagonists

The synthesis of two peptide mimetics of RGD, α-Tfm-Arg-Gly-Asp-Phe-NH₂ 9 and α-Tfm-Arg-Gly-Asp-NH-(CH₂)₂-C₆H₅ 13, is described. The precursor of α-Tfm-ornithine was obtained in two synthetic steps from 2-N-Cbz-2-Tfm-hexanediacid-1-alkyl ester and introduced into the peptide chain by α-carboxy-group activation via oxazolone. The introduction of the guanidine residue led to the final peptides as mixtures of the two diastereomers. Configurationally pure peptides were obtained in good yields by RP-HPLC.     

Synthesis of glycosyl disulfides containing an α-glycosidic linkage

A wide range of symmetrical and unsymmetrical glycosyl disulfides is synthesized with focus on the use of α-glycosyl thiols. Oxidation of α-glycosyl thiols with iodine leads to symmetrical α,α-glycosyl disulfides, while unsymmetrical disulfides are readily synthesized from α- and β-glycosyl thiols under the action of DDQ. Thus, glycosyl disulfides containing at least one α-glycosidic linkage are made available.     

Insertion of cyclopropanes between a carbonyl carbon and an α-carbon of carbonyl compounds with cyclopropylmagnesium carbenoids

The reaction of the lithium enolates of α-aryl carbonyl compounds with cyclopropylmagnesium carbenoids, derived from 1-chlorocyclopropyl p-tolyl sulfoxides with i-PrMgCl at low temperature, resulted in the formation of β-aryl carbonyl compounds bearing a cyclopropane ring at the α-position with one-carbon homologation in variable yields. The reaction was found to be highly stereospecific with respect to the stereochemistry of the cyclopropylmagnesium carbenoids. Mechanism and origin of the stereospecificity of the reaction are also discussed. This is the first example for the insertion of cyclopropanes in between a carbonyl carbon and an α-carbon of carbonyl compounds.     

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.     

Generation and cyclization of α-diazocarbothioimidates. Synthesis and structure of derivatives of 5-mercapto-1,2,3-triazole

The reaction of 5-amino-1,2,3-thiadiazol-4-carbothioamides with methyl iodide basically generates -diazo-S-methylthioimidates and -carbothioimidolates. It is shown that the reactivity of the latter increases when either alkyl or aryl substituents are introduced at the nitrogen atom of the carbothioamide groupTranslated from Khimiya Geterotsiklicheskikh Soedinenii, No. 7, pp. 979–984, July, 1992.     

Synthesis of α-alkoxyalkyltributyllead compounds via the reaction of tributylplumbyllithium with α-chloroethers,and the conjugate addition of tributylplumbyllithium to enones

α-Alkoxyalkyltributylleads 1 were prepared from the reaction of tributylplumbyllithium with α-chloroethers 2. This procedure is more convenient than the conventional method which involves transmetallation from the corresponding α-alkoxyalkyltrialkyltin. Tributylplumbyllithium was also used for the synthesis of β-oxo-organolead 4.     

Synthetic efforts towards the synthesis of fluorinated C-glycosidic analogues of α-galactosylceramides

An overview of the work realized by the group regarding the synthesis of fluorinated C-glycosides is described. The various strategies that were investigated allowed the synthesis of CF₂-glycosides for many carbohydrate series (glucose, mannose and galactose) and for any pseudo-anomeric center configuration (α or β). This work culminated in an efficient preparation of a synthetically useful α-CF₂-galactoside intermediate and its conversion to α-CF₂-galactoconjugates. A synthesis of α-CF₂-galactosylceramide, based on this last methodology, is currently investigated.     

Synthesis of a versatile building block for the preparation of 6-N-derivatized α-galactosyl ceramides: rapid access to biologically active glycolipids

A concise route to the 6-azido-6-deoxy-α-galactosyl-phytosphingosine derivative 9 is reported. Orthogonal protection of the two amino groups allows elaboration of 9 into a range of 6-N-derivatized α-galactosyl ceramides by late-stage introduction of the acyl chain of the ceramide and the 6-N-group in the sugar headgroup. Biologically active glycolipids 6 and 8 have been synthesized to illustrate the applicability of the approach.     

Synthesis of α,α-disubstituted 4-phosphonophenylalanine analogues as conformationally-constrained phosphotyrosyl mimetics

Syntheses of N-Boc (S)-4-(diethylphosphono)-(α-methyl)phenylalanine [Boc-(α-Me)Phe(4-PO₃Et₂)-OH] (9) and N-Boc (S)-2-amino-6-(diethylphosphono)tetralin-2-carboxylic acid [Boc-Atc(6-PO₃Et₂)-OH] (18) are reported as conformationally-constrained phosphotyrosyl mimetics suitably protected for peptide synthesis. Both syntheses proceeded through chiral arylhalides that are converted to arylphosphonates by palladium-catalyzed cross coupling with diethylphosphite. These amino acid analogues may be useful in the study of cellular signal transduction processes.     

Spirodiketopiperazines of mannofuranose: carbopeptoid α-amino acid esters at the anomeric position of mannofuranose

Epimeric mannofuranose anomeric aminoesters are prepared from readily available azidolactones and can act as building blocks for the incorporation of mannofuranose units into peptide chains [carbopeptoids]; alternative acylating conditions allow either rapid acylation of the more stable but kinetically hindered amine or reaction with the less hindered but less stable amine to allow control of the anomeric configuration of the products. This is exemplified by coupling of the aminoesters with glycine derivatives to give dipeptide equivalents, and subsequent cyclization to spiro diketopiperazines. Anomers with the nitrogen function cis to the 2,3-diol are more stable than those with nitrogen trans; mannofuranose derivatives are more stable than the mannopyranose isomers.     

Regioselective addtion of 5-amino-3-benzylthio-l,2,4-triazole and its analogues with aryl isocyanates

The orientation of the addition of 5-amino-3-benzylthio-1,2,4-triazole and its analogues (pyrazole) (1) with the aryl isocyanate can be directed by controlling the reaction temperature and one of the product, 5-amino-1-arylaminocarbonyl-3-benzylthio-1,2,4-triazole (pyrazole) (2), can rearrange at 170C to another product, 5-arylureylene-3-benzylthio-1,2,4-triazole (pyrazole) (3). A plausible mechanism explanation for this rearrangement reaction was presented. It was suggested that the rearrangement reaction could be referred to the thermodynamics transposition leading to the predominant 5-arylureylene-3-benzylthio-1,2,4-triazole energy preferentially.