Synthesis of monomers containing guanine or guanine precursors as substituent groups

The synthesis of four new monomers containing guanine or a guanine precursor was achieved. These were two isomeric acid ester derivatives of guanine and two isomeric vinyl ether derivatives of N²-acetylguanine. In the case of the synthesis of the guanine acid esters IV and V, it was necessary to prepare first the guanine alcohol derivatives II and III. These N-7 and N-9 isomeric alcohols of guanine were separated by fractional crystallization. Subsequent esterification of these alcohols with maleic anhydride gave the desired products. In the other case, N²-acetylguanine was alkylated with 2-chloroethyl vinyl ether to yield the N-7 and N-9 isomer VI and VII, respectively. These were separated using flash column chromatography.     

Synthesis of Derivatives of ω-Isocyanato-α-methylamino, ω-Ureido-α-methylamino, and Nα-Methyl-α, ω-diamino Acids

 Homochiral N^α-methyl-2,3-diaminopropionic and N^α-methyl-2,4-diaminobutyric acid derivatives 8a,b were obtained via a stereoconservative four-step synthesis starting from hexafluoroacetone protected L-aspartic and L-glutamic acid 2a,b, respectively. Hexafluoroacetone protected ω-isocyanato-α-methylamino acids 4a,b– the key intermediates of the synthesis – are versatile building blocks for amino acid and peptide modification and promising candidates for combinatorial chemistry. Upon reaction with alcohols, compounds 4 give activated N ^ω-urethane protected ω-amino-α-methylamino acid derivatives 5–7; upon reaction with amines, ω-ureido-α-methylamino acid derivatives 10–12 and 3-methylamino-pyrrolidin-2-ones 13 are available.     

Synthesis of Derivatives of ω-Isocyanato-α-methylamino, ω-Ureido-α-methylamino,and N<Superscript>α</Superscript>-Methyl-α, ω-diamino Acids

Summary.  Homochiral N^α-methyl-2,3-diaminopropionic and N^α-methyl-2,4-diaminobutyric acid derivatives 8a,b were obtained via a stereoconservative four-step synthesis starting from hexafluoroacetone protected L-aspartic and L-glutamic acid 2a,b, respectively. Hexafluoroacetone protected ω-isocyanato-α-methylamino acids 4a,b– the key intermediates of the synthesis – are versatile building blocks for amino acid and peptide modification and promising candidates for combinatorial chemistry. Upon reaction with alcohols, compounds 4 give activated N ^ω-urethane protected ω-amino-α-methylamino acid derivatives 5–7; upon reaction with amines, ω-ureido-α-methylamino acid derivatives 10–12 and 3-methylamino-pyrrolidin-2-ones 13 are available. Received November 17, 1999. Accepted November 26, 1999     

Syntheses of Peptidoglycolipid Analogs with Distinct Immunomodulating Activities

ABSTRACT

Amphiphilic 2-amino-2-deoxy-β-D-glucopyranosylamides were synthesized from N-protected glucosamine derivatives via N-glycosidation with fatty amines, subsequent N-acylation with fatty acid derivatives and deprotection. They could further be modified with amino acids to give peptido-glycopyranosyl amides, some of which exhibited strong immunostimulatory (BAY Q8939, 8) or immunoadjuvant (BAY R1005, 9) activities.     

Diels-alder reactions of 2- and 3-vinyl-1-(phenylsulfonyl)pyrroles

Regioselectively produced 2- and 3-acetyl-1-(phenylsulfonyl)pyrroles can be reduced to the corresponding alcohols and subsequently dehydrated to afford N-protected vinylpyrroles. These remarkably stable vinylpyrroles can then serve as heterodienes in [4 + 2] cycloaddition reactions with electron deficient dienophiles to afford tetrahydroindole derivatives.     

Synthesis of Amino Acid Derivatives of Neamine and 2-Deoxystreptamine to be used as Mutasynthons

ABSTRACT

6′-N derivatives of neamine with alanine, phenylalanine and lysine were synthesized either using an active esters method in one step under controlled conditions, or using a mixed anhydride method after blocking every functional group of neamine and leaving the 6′-amino group free to react. Similarly N,N′-diamino acid and monoamino acid derivatives of 2-deoxystreptamine were synthesized.     

Alcohols and aluminium alkoxides in the presence of raney nickel as alkylating agents. 1. Alkylation of indoles and pyrroles

Indole and 3-methylindole are completely converted by alcohols into N-alkyl or N-isoalkyl derivatives in the presence of aluminium alkoxides and Raney Nickel; 2-methylindole gives lower yields. Pyrroles suffer N- and C-alkylation but the initially formed N-alkylpyrroles are reduced into N-alkylpyrrolidines in the reaction mixtures. The occurrence of these N-alkylations is at variance with the C-alkylation of indoles and pyrroles which takes place by means of alcohols and sodium alkoxides. This suggests that the reaction occurs between the substrate and the reagent both coordinated by aluminium.     

PREPARATION OF FORMIC ACID ESTERS WITH A PHOSPHONIUM SALT AND ZINC BROMIDE IN N,N-DIMETHYLFORMAMIDE

ABSTRACT

When primary and secondary alcohols were treated with the phosphonium salt 1 and ZnBr₂ in N,N-dimethylformamide, the corresponding formic acid esters were obtained in good yields.     

Cu‐Catalyzed Aerobic Oxidative Cyclizations of 3‐N‐Hydroxyamino‐1,2‐propadienes with Alcohols,Thiols, and Amines To Form α‐O‐, S‐, and N‐Substituted 4‐Methylquinoline Derivatives

A one‐pot, two‐step synthesis of α‐O‐, S‐, and N‐substituted 4‐methylquinoline derivatives through Cu‐catalyzed aerobic oxidations of N‐hydroxyaminoallenes with alcohols, thiols, and amines is described. This reaction sequence involves an initial oxidation of N‐hydroxyaminoallenes with NuH (Nu=OH, OR, NHR, and SR) to form 3‐substituted 2‐en‐1‐ones, followed by Brønsted acid catalyzed intramolecular cyclizations of the resulting products. Our mechanistic analysis suggests that the reactions proceed through a radical‐type mechanism rather than a typical nitrone‐intermediate route. The utility of this new Cu‐catalyzed reaction is shown by its applicability to the synthesis of several 2‐amino‐4‐methylquinoline derivatives, which are known to be key precursors to several bioactive molecules.     

Direct Synthesis of Z,Boc, Fmoc,Alloc[ddot] Derivatives of 5-Aminooxazoles Starting from Acylamino Acids and Chlorosulfonylcarbamates

A one-step synthesis of 5-oxazolecarbamates 1–11 can be easily carried out starting from N-acetylated and benzoylated aminoacids such as Gly, Ala, Leu, Phe, and chlorosulfonyl carbamates, prepared in situ by addition of alcohols on chlorosulfonyl isocyanate (CSI). The structure of the compounds was confirmed by X-Ray crystallography. A subsequent exocyclic N-alkylation gave substituted 12–18 derivatives. Carbamate cleavage gave by spontaneous reopening substituted N-acylaminoamides, in excellent yields.     

Highly Chemoselective gem-Difluoropropargylation of Aliphatic Alcohols

Despite the potential of α-fluoroethers in medicinal chemistry, their synthetic methods, especially etherification of aliphatic alcohols, have been limited. Herein, we developed two- and three-step gem-difluoropropargylation of aliphatic alcohols including amino acid derivatives and naturally occurring bioactive molecules. Highly chemoselective etherification proceeded by using the gem-difluoropropargyl bromide dicobalt complex in the presence of silver triflate and triethylamine. Decomplexation of dicobalt complexes was achieved by using cerium ammonium nitrate or N,N,N′-trimethylethylenediamine. The thus obtained gem-difluoropropargyl ethers were converted to various α-difluoroethers which are expected to be useful for medicinal chemistry.     

Pyrazoles and Pyrazolo[4,3- e]pyrrolo[1,2- a]pyrazines, I. Synthesis and Antimicrobial Activity

The synthesis of the title compounds was achieved using 1-phenyl-5-(pyrrol-1-yl)-1H-pyrazole-3-carboxylic acid azide as starting material. The latter compound was allowed to react with alcohols and amines to afford the corresponding carbamates and urea derivatives. Alkaline hydrolysis of the carbamates gave the corresponding amine, which was acylated and/or aroylated to give amide derivatives. These and the urea derivatives were subjected to cyclodehydration to give the title compounds. Antibacterial and antifungal activities were observed for several derivatives.     

Conventional and Microwave Assisted Hydrogenolysis Using Zinc and Ammonium Formate

Abstract

The selective deprotection of several N‐Bzl amino derivatives to the corresponding amines and the removal of S‐Bzl and O‐Bzl groups from the protected amino acids with ammonium formate and commercial zinc dust are reported. Many other reducible or hydrogenolysable substituents such as halogens, methoxy, phenol, ester, acid, ethene, and Boc groups are unaffected.     

Further studies on homopolymers and copolymers resulting from the reaction of polymaleic anhydride with alcohols and amines

Polymaleic anhydride prepared by γ-rays irradiation of maleic anhydride was used as a reactive polymer and reacted with certain long-chain aliphatic amines and/or alcohols as well as with the mesogenic biphenylamine. The homopolymers and copolymers that were prepared, i.e., derivatives of N-alkyl polymaleamic acid, monoesters of polymaleic acid, or mixed amide-ester derivatives, were primarily investigated as far as their property to show thermotropic liquid crystalline character is concerned. By this investigation the structural features for the exhibition of mesomorphism by these polymers were determined.     

Pyrazoles and Pyrazolo[4,3-<Emphasis Type="Italic">e</Emphasis>]pyrrolo[1,2-<Emphasis Type="Italic">a</Emphasis>]pyrazines,I. Synthesis and Antimicrobial Activity

Summary. The synthesis of the title compounds was achieved using 1-phenyl-5-(pyrrol-1-yl)-1H-pyrazole-3-carboxylic acid azide as starting material. The latter compound was allowed to react with alcohols and amines to afford the corresponding carbamates and urea derivatives. Alkaline hydrolysis of the carbamates gave the corresponding amine, which was acylated and/or aroylated to give amide derivatives. These and the urea derivatives were subjected to cyclodehydration to give the title compounds. Antibacterial and antifungal activities were observed for several derivatives.     

A Practical Synthesis of ω-Aminoalkanoic Acid Derivatives from Cycloalkanones

A practical synthetic route to N-Boc protected or Boc-amino acid coupled ω-aminoalkanoic acids is reported and exemplified by the preparation of 8-(t-butoxycarbonylamino)caprylic acid 2 and (N-t-butoxycarbonylphenylalanyl)-8-aminocaprylic acid 3. The sequence does not involve column chromatography, hydrogenation, azide or bromine related rearrangements, and therefore is amenable to scale-up. Homologues of the ω-aminoalkanoic acid derivatives may also be prepared by using different cycloalkanones.     

Facile Synthesis of Nicotinic Acid Derivatives with Unsymmetrical Substitution Patterns

Abstract

Two novel methods for synthesis of nicotinic acid derivatives with unsymmetrical substitution patterns were presented via ketene dithioacetals. The ketene N,S-acetals 2 reacted with β-ketoesters or β-cyanoesters to give 4-amino-5-cyano-2-alkyl-6-methylthio-nicotinic acid derivatives 3 or 2,4-diamino-5-cyano-6-methylthio-nicotinic acid ethyl ester 4. However, 6-amino-5-cyano-2-alkyl-4-methylthio-nicotinic acid esters 6 were obtained by the reaction of the ketene dithioacetals 1 and β-amino-crotonates.     

Functionalization and cyclization reactions of 4-benzoyl-1,5-diphenyl- 1H-pyrazole-3-carboxylic acid

The 1H-pyrazole-3-carboxylic acid 2 or its remarkably stable acid chloride 3 can easily be converted into the corresponding ester or amide derivatives 4 or 5, respectively, from reaction with alcohols or N-nucleophiles. Pyrazolo[3,4-d]pyridazines 6a,b are obtained from cyclocondensation reactions of the pyrazoles 2 and 3, respectively, with phenylhydrazine or hydrazine hydrate, while 6c is formed in an one-pot procedure from the furan-2,3-dione 1 and hydrazine hydrate.     

Regioselective synthesis of 2,4-disubstituted thiophenes

A highly regioselective route was established to 2-aryl-, 2-cyclohexyl-, and 2-(2-arylethyl)4-alkylthiophenes, which are potential candidates as liquid crystalline compounds of low viscosity. The key synthetic intermediates, 2-substituted-4-(chloromethyl)thiophenes 6, 14, and 20 were prepared respectively from the reactions of β, γ-epoxycarbonyl compounds 5, 13, and 19 with Lawesson's reagent in the presence of a catalytic amount of p -toluenesulfonic acid. The epoxycarbonyl compounds were obtained from the TiCl₄-mediated reactions of 2-(chloromethyl)-3-(trimethylsliyl)propene (10) with acid chlorides followed by epoxidation with m-chloroperoxybenzoic acid, or from prior epoxidation followed by oxidation with pyridinium dichromate of homoallylic alcohols 3. The homoallylic alcohols 3 were synthesized from the reactions of 2-(chloromethyl)-3-(trichlorosilyl)propene (2) with aldehydes in N, N-dimethylformamide. Copper (I) catalysed cross-coupling reactions of 2-substituted-4-(bromomethyl)thiophenes (which were prepared by transhalogenation of 2-substituted-4- (chloromethyl)thiophenes with NaBr in acetone) with Grignard reagents afforded 2,4-disubstituted thiophenes. Using this method, eleven 2,4-disubstituted thiophenes were synthesized and their potentials as liquid crystalline compound of low viscosity were examined. The synthesized 2-(4-cyanophenyl)-4-pentylthiophene was observed to have a lower melting point than the corresponding 2,5-disubstituted thiophene. This observation is consistent with the expectation from the basis of molecular linearity which can affect the viscosity and/or melting point of crystalline compounds.     

Les β-cétonitriles groupes protecteurs de la fonction amine. Préparation d'amino-alcools

β-Ketonitrile-Derived Protecting Groups of the Amino Function. Synthesis of Amino Alcohols The amino group of natural L -amino acid esters is protected by condensation with 2-oxocyclopentanenitrile ( 1 ) or 2-formyl-2-phenylacetonitrile ( 10 ). Only the ester group of the formed cyanoenamino esters 2 and 11 reacts with nucleophilic reagents such as organometallics (RMgX, RLi), borohydrides, or metal amides, whereas the cyanoenamino group is unchanged (Schemes 1 and 2). Cyanoenamino alcohols obtained by reduction of cyanoenamino esters 2 are hydrolyzed under acidic conditions to amino alcohols with retention of the configuration of the starting amino acid. This sequence of reactions allows to prepare derivatives of L -tyrosinol from (?)-L -tyrosine (see, e.g., Scheme 4). Cyanoenamino esters 11 are readily methylated at the N-atom to give N-methylated cyanoenamino esters (Scheme 3). This property is exploited on the way of a multistep procedure to obtain N-methylated amino alcohols homologous to natural (?)-(1R,2S)-ephedrine.