Synthesis of 5-aryl-2-oxazolepropionic acids and analogs. Antiinflammatory agents

Condensation of 2-bromoacetophenones with sodium succinimide gave N-phenacylsuccinimides ( 1 ) which were opened with sodium hydroxide to N-phenacylsuccinamic acids ( 2 ). The latter were cyclized to 5-aryl-2-oxazolepropionic acids ( 3 ) in sulfuric acid. Similar cyclization of N-phenacylphthalamic acid ( 5 ) and succinic acid 2-benzoylhydrazide ( 7 ) gave o-(5-phenyl-2-oxazolyl)benzoic acid ( 6 ) and 5-phenyl-1,3,4-oxadiazole-2-propionic acid ( 8 ). The succinamic acids 2 and the phthalamic acid 5 were observed to recyclize to the corresponding imides ( 1 and 4 ) on heating, and the succinic acid hydrazide 7 was similarly cyclized to N-benzamidosuccinimide ( 9 ) with acetic anhydride. Antiinflammatory screening data are reported for 3 , 6 and 8 .     

An improved synthesis of homopteroic and homofolic acids

A more practical synthesis of homopteroic and homofolic acids involving condensation of 2,4,5-triamino-6(1H)pyrimidinone ( 3 ) with 1-acetoxy-4-[N-acetyl-(p-carbethoxyphenyl)amino]-2-butanone ( 7 ) is described. The biological activities of homofolic ( 1-b ) and homopteroic ( 2-b ) acids were compared and found to be identical with the activities of these products prepared by the unambiguous route.     

Asymmetric Alkylations of a Sultam-Derived Glycine Equivalent: Practical preparation of enantiomerically pure α-amino acids

Alkylation of the chiral glycine derivative 2 with “activated” organohalides under ultrasound-assisted phasetransfer catalysis or with activated and nonactivated organohalides in anhydrous medium provides (mostly crystalline) alkylation products 3 . Acidic hydrolysis of the pure products 3 gives (aminoacyl)sultams 4 which by mild saponification furnish pure α-amino acids 5 in good overall yields from 2 , along with recovered auxiliary 1 (Scheme 1). Pure ω-protected α,ω-diamino acids and α-amino-ω-(hydroxyamino)acids 12–16 are readily accessible from (ω-haloacyl)sultams 3 via reaction with N-nucleophiles followed by acidic and basic hydrolyses (Scheme 2). A reliable determination of the enantiomeric purity of α-amino acids using HPLC analysis of their N-(3,5-dinitrobenzoyl)prolyl derivatives 17 is presented.     

Directed synthesis and immunoactive properties of (2-hydroxyethyl)ammonium salts of 1-R-indol-3-ylsulfanyl(sulfonyl)alkanecarboxylic acids

A general method for the synthesis of 1-alkyl(allyl)(benzyl)-substituted (indol-3-yl)-sulfanylalkanecarboxylic acids and hexane-1,6-diyl(1,4-phenylenemethylene)bisindol-3-ylsulfanylalkanecarboxylic acids from the corresponding N-substituted indoles and bisindoles, thiourea, iodine, and halogencarboxylic acids was developed. The oxidation of substituted (indol-3-yl)sulfanylalkanecarboxylic acids for the first time afforded their analogs containing the sulfonyl group. New (2-hydroxyethyl)ammonium salts of 1-R-indol-3-ylsulfanyl(sulfonyl)-alkanecarboxylic acids, which are structural analogs of highly active immunomodulators of indacetamin and VILIM, were synthesized. Among the studied (2-hydroxyethyl)ammonium salts of 1-R-indol-3-ylsulfanylacetic and -sulfonylalkanecarboxylic acids, the compounds exhibiting high dose-dependent antiproliferative activity by the ability to affect the spontaneous and mitogen-stimulated splenocyte proliferation of mice in vitro were found.     

Cyclic hydroxamic acids derived from quinazoliue

The action of various acylating agents on 2-aminobenzohydroxamic acid afforded 3-hydroxy-4(3H)quinazolinones (hydroxamic acids) as well as several ethers and esters from them were prepared and their spectroscopic properties analyzed. Secondary amines, as well as one equivalent of alkali, on 2-halomethyl-3-hydroxy-4(3H)quinazolinone lead to the formation of a dimer(XI). In this respect the behaviour of secondary amines is different from that of primary amines. Some new 3-hydroxy-2-4(1H,3H)-quinazolidinediones are described.     

Phase transitions in molecular crystals of carboxylic acids

A comparative analysis of phase transitions in molecular crystals of carboxylic acids (n-alkano acids) with various chain lengths, (CH₃(CH₂) _n COOH) is performed with the use of DSC. A number of new effects related to first-order phase transitions are discovered. The temperature dependence of heat capacity is quantitatively analyzed in terms of the theory of blurred (Λ-shaped) phase transitions of the first order.     

Synthesis and anticancer activity evaluation of 3-(4-oxo-2-thioxothiazolidin-5-yl)-1H-indole-carboxylic acids derivatives

Abstract

A mild and efficient method for the synthesis of 1-oxo-9H-thiopyrano[3,4-b]indole-3-carboxylic acids and dimerized 3-(4-carboxy-1H-3-indolyl)-2-propenoic acids via alkaline hydrolysis of 3-(rhodanin-5-yl)-1H-indole-2-carboxylic acids derivatives was elaborated. Anticancer activity screening in NCI60-cell lines assay allowed identification of 5-fluoro-3-(4-oxo-2-thioxothiazolidin-5-ylidenemethyl)-1H-indole-2-carboxylic acid methyl ester 2a with significant antimitotic activity at micromolar and submicromolar concentrations.     

Cyclic imides III. A study of the hydroxy- and methoxyphthalimidoacetic acids and the methyl methoxyphthalimidoacetates

The hydroxy- and methoxyphthalimidoacetic acids and the methyl methoxyphthalimidoacetates have been synthesized. The ultraviolet absorption spectra of these compounds in 95% ethanol, aqueous acid, and aqueous base are discussed. Structures are suggested for the hydroxy- and methoxyphthalamate ions which are formed in basic solution. The Gabriel-Colman rearrangements of methyl 3- and 4 - methoxyphthalimidoacetate give, respectively, 8-methoxy-4-hydroxy-3 - carbomethoxy-1(2H)-isoquinolone (VII) and 6-methoxy-4-hydroxy-3-carbomethoxy-1(2H)-isoquinolone (VIII).     

Determination of amino acids by gas chromatography using a wide bore capillary column

A procedure is described in which a wide bore capillary column is used as an alternative to the more traditional packed column for the quantitative analysis of amino acids as their N-heptafluorobutyryl isobutyl ester (HBB) derivatives. The column, installed in a gas chromatograph previously configured for use with a packed column, is shown to give good reproducibility by repeated determination of amino acid response factors (RSD values for all amino acids are below 3%). A number of problems, encountered during the use of this column, are discussed and suitable techniques to overcome them are reported.     

Investigation and radiometric determination of saturated and unsaturated aliphatic monocarboxylic acids and aromatic dicarboxylic acids

Investigations have been carried out on the precipitation of calcium salts of saturated and unsaturated aliphatic monocarboxylic acids and of aromatic dicarboxylic acids. The optimum ethanol/water solvent ratio has been studied at which the sodium, ammonium or triethylammonium salts of the acids have a good solubility, whereas the calcium salts are poorly soluble and can be precipitated. Based on these investigations the radiometric determination of formic acid, palmitic acid, stearic acid, methacrylic acid, oleic acid, and o-, m- and p-phthalic acids has become possible. A linear correlation has been found between the solubilities of the calcium salts of o-, m- and p-phthalic acids and the dielectric constant of the solvent mixture. CaCl₂ solution labelled with⁴⁵CaCl₂ was used for the titrations, with a solvent composition identical to that of the solution to be titrated. Radiometric titrations were carried out in 0.05M solutions for dicarboxylic acids, and in 0.1M solutions for monocarboxylic acids. For palmitic and stearic acids titrations were also carried out in the 0.01M concentration range. The equipment used for titrations was capable of detecting isotopes of soft β-radiation.     

Fatty acids from the Okhotsk sea sponge <Emphasis Type="Italic">Forcepia uschakowi</Emphasis>

The fatty-acid (FA) composition of total lipids from the Okhotsk sea marine sponge Forcepia uschakowi was studied. A total of 56 acids were identified by GC and GC—MS. The principal saturated acids were 16∶0 and 18∶0. The main monoene acid was 15-Me-24∶1(14), which was observed for the first time in sponge lipids. Polyunsaturated acids represented of 64.1% of the total FA of F. uschakowi. Of these, the principal ones were non-methylene-separated acids 26∶2(5,9) and 26∶3(5,9,19), which are typical of sponges, and bromo-acid 6-Br-26∶2(5,9). __________ Translated from Khimiya Prirodnykh Soedinenii, No. 5, pp. 422–424, September–October, 2007.     

17O NMR spectroscopy: Effect of substituents on chemical shifts for p-substituted benzoic acids,methyl benzoates,cinnamic acids and methyl cinnamates

The ¹⁷O NMR spectra for a series of ¹⁷O-enriched p-substituted benzoic acids, methyl benzoates, cinnamic acids and methyl cinnamates in acetone at 40°C are reported. The carboxylic acids showed one signal (benzoic 250.5 ppm, SCS range p-MeO to p-NO₂ = 10.5 ppm; cinnamic 254.1 ppm, SCS range p-MeO to p-NO₂ = 5.4 ppm). The esters showed two signals [methyl benzoate (C?O) 341.3 ppm and (OCH₃) 128.0 ppm; methyl cinnamate (C?O) 339.9 ppm and (OCH₃) 134.2 ppm]. The SCS ranges for the carbonyls of the esters were larger than those for the corresponding acids, while those for the OCH₃ groups of the esters were slightly smaller. The carbonyl data gave good correlations with σ⁺ constants, while the OCH₃ data gave at best only a poor correlation with σ constants. Dual substituent parameter treatment improved the correlations for all the data using σ_R+ constants. The ratios of ρ_I to ρ_R+ were similar for all the sets of data.     

Synthesis of asymmetric cyclopropyl acids and amines

(+) (S)- and (?) (R)-trans-1,2-cyclopropanedicarboxylic acids (C3A), (+) (S)- and (?) (R)-trans-1,2-diaminocyclopropanes (C3B), (+) (S)- and (?) (R)-trans-2-phenylcyclopropylamines (øC3B), (+) (S)- and (?) (R)-trans-1,2-bis(methylamino)-cyclopropanes (C3MB), and (+) (S)- and (?) (R)-trans-(2-phenylcyclopropyl)-methylamines (øC3MB) were prepared.     

Synthesis of novel amphiphilic pyridinylboronic acids

Novel 3‐alkoxy‐2‐pyridinylboronic acids bearing, in their 3‐position, linear alkoxy or perfluoroalkoxy chains with n carbon atoms (n = 6, 8, 10, 12 and 18) 2a – 2g are synthesized from 2‐bromo‐3‐pyridinol, which is the common starting product. Our alternative procedure for the synthesis of 3‐alkoxy‐2‐bromopyridine in a phase‐transfer catalysis system is to carry out the reaction in a solid–liquid medium in the presence of a quaternary ammonium salt under microwave irradiation. General and versatile synthetic methods have been developed for preparation of a large variety of new 2‐pyridinylboronic acids bearing two alkylated or perfluoroalkylated side chains with an ether junction in the 3‐position. Copyright © 2003 John Wiley & Sons, Ltd.     

Synthesis of 5-methyl-4-oxo-quinolinecarboxylic acids

A series of 5-methyl-4-oxo-3-quinolinecarboxylic acids was prepared in which the eight-position was substituted with fluorine, chlorine, methyl, or hydrogen. These quinolones were synthesized from the appropriate 2-methyl-3,4,6-trifluorobenzoic acids which were derived from oxazolines 8 and 16 . The oxazoline moiety served as both an ortho-director (where feasible) and a protecting group; a trimethylsilyl moiety was used to block the most acidic site in the molecule.     

Access to the 2,3-dihydropyridazin-3-one and as-triazino[3,4-a]phthalazine ring systems from 4-aryl-2-oxo-butanoic acids

A novel series of 2,3-dihydropyridazin-3-ones 15 were synthesized via condensation between hydrazines and 4-(p-chlorophenyl)-2-hydroxy-2-(2-oxo-2-substituted ethyl)butanoic acids 8 which in turn were prepared by the reaction of substituted benzylpyruvic acids 6 with methyl alkyl(aryl) ketones 7. Dehydration of 8b-d by a mixture of glacial acetic acid and hydrochloric acid afforded 4-(p-chorophenyl)-2-(substituted phenacyl)-2-butenoic acids 10. Condensation reaction of 10 with hydrazines gave type 15 compounds in good yields. Also, a new series of as-triazino[3,4-a]phthalazines 20 was obtained from the reaction of substituted benzylpyruvic acids 6 with hydralazine to give the hydralazones 19 which underwent dehydrative cyclization reaction with PPA to afford 20. Structure assignments are based on ¹H, ¹³C nmr and ir spectra.     

Preparation and some properties of maleimido acids and maleoyl derivatives of peptides.

N-Alkoxycarbonylmaleimides 3 have been prepared and used to convert amino acids to maleimido acids (6–8) in aqueous solution. The carboxyl group of maleimido acids can be activated for amide or peptide synthesis (e.g., in the N-succinimidyl esters 10); t-butyl-based protecting groups can be cleaved without damage to the maleimide moiety. Peptides carrying maleimide groups are accessible either from the maleimido acids (e.g., 11b, 15) or by direct maleoylation (e.g., 16b). The maleoyl group can be cleaved off by successive mild alkaline and acid hydrolysis or by hydrazinolysis. The reactivity of maleimides toward thiol groups suggests the use of maleimido acids and maleoylpeptides for preparing a wide range of conjugates of biochemical interest.     

ESI‐MS/MS analysis of protonated N‐methyl amino acids and their immonium ions

Methylation is one of the important posttranslational modifications of biological systems. At the metabolite level, the methylation process is expected to convert bioactive compounds such as amino acids, fatty acids, lipids, sugars, and other organic acids into their methylated forms. A few of the methylated amino acids are identified and have been proved as potential biomarkers for several metabolic disorders by using mass spectrometry–based metabolomics workstation. As it is possible to encounter all the N‐methyl forms of the proteinogenic amino acids in plant/biological systems, it is essential to have analytical data of all N‐methyl amino acids for their detection and identification. In earlier studies, we have reported the ESI‐MS/MS data of all methylated proteinogenic amino acids, except that of mono‐N‐methyl amino acids. In this study, the N‐methyl amino acids of all the amino acids ( 1 ‐ 21 ; including one isomeric pair) were synthesized and characterized by ESI‐MS/MS, LC/MS/MS, and HRMS. These data could be useful for detection and identification of N‐methyl amino acids in biological systems for future metabolomics studies. The MS/MS spectra of [M + H]⁺ ions of most N‐methyl amino acids showed respective immonium ions by the loss of (H₂O, CO). The other most common product ions detected were [MH‐(NH₂CH₃]⁺, [MH‐(RH)]⁺ (where R = side chain group) ions, and the selective structure indicative product ions due to side chain and N‐methyl group. The isomeric/isobaric N‐methyl amino acids could easily be differentiated by their distinct MS/MS spectra. Further, the MS/MS of immonium ions inferred side chain structure and methyl group on α‐nitrogen of the N‐methyl amino acids.     

Structural characterization of monohydroxyeicosatetraenoic acids and dihydroxy- and trihydroxyeicosatrienoic acids by ESI-FTICR

The fragmentation characteristics of monohydroxyeicosatetraenoic acids and dihydroxy- and trihydroxyeicosatrienoic acids were investigated by electrospray ionization Fourier transform ion cyclotron resonance (FTICR) mass spectrometry using sustained off-resonance irradiation collision-induced dissociation (SORI-CID) and infrared multiphoton dissociation (IRMPD). The fragmentation patterns of these compounds were associated with the number and positions of the hydroxyl substituents. The fragmentation is more complicated with increasing number of the hydroxyl groups of the compounds. In general, the major carbon-carbon cleavage of [M−H]⁻ ions occurred at the α-position to the hydroxyl group, and the carbon-carbon cleavage occurred when there was a double-bond at the β-position to the hydroxyl group. SORI-CID and IRMPD produced some common fragmentation patterns; however, each technique provided some unique patterns that are useful for structural identification of these compounds. This study demonstrated the application of FTICR via the identification of regioisomers of trihydroxyeicosatrienoic acids in rabbit aorta samples.     

Synthesis of alkylaminoethanethiolsulfuric acids substituted with heterocyclic moieties

Several alkylaminoethanethiolsulfurie acids substituted with heterocyclic moieties have been synthesized to determine their effectiveness as radiation protection agents. These compounds are represented by the structure R(CH₂)₃NH(CH₂)₂S₂O₃H, where R is 8-quinoly-oxy (V), 8-quinaldyloxy (IX), 5-quinolyloxy (XII), 4-pyridyl (XVI), and 4-pyridylmethyl (XXIII). The diheterocyclic-substituted compound, 2-[bis-(2-phenyl-1, 2, 3, 2H-triazol-4-ylmethyl)amino]ethanethiolsulfuric acid (XIV) was also synthesized.