Regioselective 1,3‐Dipolar Cycloadditions of (1Z)‐1‐(Arylmethylidene)‐5,5‐dimethyl‐3‐oxopyrazolidin‐1‐ium‐2‐ide Azomethine Imines to Acetylenic Dipolarophiles

The 5,5‐dimethylpyrazolidin‐3‐one ( 4 ), prepared from ethyl 3‐methylbut‐2‐enoate ( 3 ) and hydrazine hydrate, was treated with various substituted benzaldehydes 5a – i to give the corresponding (1Z)‐1‐(arylmethylidene)‐5,5‐dimethyl‐3‐oxopyrazolidin‐1‐ium‐2‐ide azomethine imines 6a – i . The 1,3‐dipolar cycloaddition reactions of azomethine imines 6a – h with dimethyl acetylenedicarboxylate (=dimethyl but‐2‐ynedioate; 7 ) afforded the corresponding dimethyl pyrazolo[1,2‐a]pyrazoledicarboxylates 8a – h , while by cycloaddition of 6 with methyl propiolate (=methyl prop‐2‐ynoate; 9 ), regioisomeric methyl pyrazolo[1,2‐a]pyrazolemonocarboxylates 10 and 11 were obtained. The regioselectivity of cycloadditions of azomethine imines 6a – i with methyl propiolate ( 9 ) was influenced by the substituents on the aryl residue. Thus, azomethine imines 6a – e derived from benzaldehydes 5a – e with a single substituent or without a substituent at the ortho‐positions in the aryl residue, led to mixtures of regioisomers 10a – e and 11a – e . Azomethine imines 6f – i derived from 2,6‐disubstituted benzaldehydes 5f – i gave single regioisomers 10f – i .     

Purines. Part XVI

A series of N‐substituted 8‐aminoxanthines (=8‐amino‐3,7(or 3,9)‐dihydro‐1H‐purine‐2,6‐diones) 8 – 16 and 34 – 37 were synthesized from the corresponding 8‐nitroxanthines 1 – 7, 30 – 33 , and 8‐(phenylazo)xanthines 17 and 18 by catalytic reduction. Another approach was derived from 6‐amino‐5‐(cyanoamino)uracils (=N‐(6‐amino‐1,2,3,4‐tetrahydro‐2,4‐dioxopyrimidin‐5‐yl)cyanamides) 23, 24 , and 27 by base‐catalyzed cyclization yielding 25 – 28 . All 8‐aminoxanthines 8 – 29 and 34 – 37 were acetylated to the corresponding 8‐(acetylamino)xanthines 40 – 57 , and prolonged heating led to 8‐(diacetylamino)xanthines 58 and 59 . Several 8‐aminoxanthines 8 – 13 were diazotized forming 8‐diazoxanthines 60 – 64 . Coupling reactions of isolated 62 and 64 and intermediary formed 8‐diazoxanthines with 1,3‐dimethylbarbituric acid (=1,3‐dimethylpyrimidine‐2,4,6(1H,3H,5H)‐trione; 66 ) resulted in 5‐[(xanthin‐8‐yl)diazenyl]‐1,3‐dimethylbarbituric acids=3,7(or 3,9)‐dihydro‐8‐[2‐(1,2,3,4‐tetrahydro‐1,3‐dimethyl‐2,4‐dioxopyrimidin‐5‐yl)diazenyl]‐1H‐purine‐2,6‐diones) 67 – 80 . The newly synthesized xanthine derivatives were characterized by the determination of their pK_a values, the UV‐ and NMR spectra, as well as elemental analyses.     

Triarylborane-Appended Anils and Boranils: Solid-State Emission,Mechanofluorochromism, and Phosphorescence

Herein, the design, synthesis, optical properties, and mechanofluorochromism characteristics of a series of conjugates having covalently linked triarylborane (TAB) and anil/boranil units (TAB-anil: 1 a – 3 a and TAB-boranil: 1 – 3 ) are reported. The electronic interactions between TAB and anil/boranil in 1 a – 3 a and 1 – 3 were fine-tuned by changing the boryl moiety's position on the phenyl spacer connecting the BMes₂ (Mes=mesityl) and anil/boranil units. A boryl moiety at the meta position ( 1 a ) of the phenyl spacer stabilizes the enolic form (E-OH), whereas a boryl moiety at the para position ( 2 a and 3 a ) stabilizes the keto form (Z-NH) in the solid state. However, in solution 1 a , 2 a , and 3 a exhibit keto–enol tautomerism in both ground and excited states. Compounds 1 a – 3 a and 1 – 3 show red-shifted absorption compared with 4 a and 4 , which are devoid of TAB moieties, which indicate effective participation of an empty p orbital on the boron center in 1 a – 3 a and 1 – 3 . Compounds 1 and 2 showed fluorescence variations in response to external stimuli such as mechanical grinding. Long phosphorescence lifetimes of 18–46 ms were observed for compounds 1 – 3 . The observed optical properties of 1 a – 3 a and 1 – 3 are rationalized in the context of quantum mechanical calculations.     

7-Halogenated 7-Deaza-2′-deoxyinosines

The synthesis of the 7-deaza-2′-deoxyinosine derivatives 3a – c with chloro, bromo, and iodo substituents at position 7 is described. Glycosylation of the 7-halogenated 6-chloro-7-deazapurines 4a – c or of the 7-halogenated 6-chloro-7-deaza-2-(methylthio)purines 9a – c with 2-deoxy-3,5-di-O-(4-toluoyl)-α-D -erythro-pentofuranosyl chloride ( 5 ) furnished the intermediates 7a – c and 11a – c , respectively, which gave, upon deprotection, the desired nucleosides 3a – c .     

Effects of different basis sets and donor‐acceptor groups on linear and second‐order nonlinear optical properties and molecular frontier orbital energies

The calculation of molecular hyperpolarizability, molecular frontier orbital energies of some donor‐acceptor oxadiazoles ( 5a – f , 8a – f , and 9a – f ) have been investigated using ab initio methods and different basis sets. Ab initio optimizations were performed at the Hartree–Fock (HF) and density functional (Beckee‐3–Lee–Yang–Parr; B3LYP) levels of theory with 6‐31G basis set. The polarizability (<α>), anisotropy of polarizability (Δα), and ground‐state dipole moment (μ), first hyperpolarizability (β), and molecular frontier orbital (HOMO, highest occupied molecular orbital and LUMO, lowest unoccupied molecular orbital) energies of 5a – f , 8a – f , and 9a – f have been calculated at the HF and B3LYP methods with 6‐31G, 6‐31G(d), 6‐31+G(d), 6‐31++G(d,p), 6‐311G, 6‐311G(d), 6‐311+G(d), and 6‐311++G(d,p) basis sets. Also, the molecular hardness (η) and electronegativity (χ) parameters have been obtained using molecular frontier orbital energies. The <α>, Δα, μ, β, HOMO, LUMO energies, η and χ parameters have been investigated as dependence on the choice of method and basis set. The variation graphics of <α>, Δα, μ, β, η, and χ parameters using HF and B3LYP methods with different basis sets are presented. We have examined the frontier molecular orbital pictures of 5a – f , 8a – f , and 9a – f using B3LYP/6‐31++G(d,p) level. The 5a – f , 8a – f , and 9a – f display significant linear, second‐order molecular nonlinearity, and molecular parameters and provide the basis for future design of efficient nonlinear optical materials having the 1,3,4‐oxadiazole core. © 2009 Wiley Periodicals, Inc. Int J Quantum Chem, 2011     

Syntheses of the Macrocyclic Spermine Alkaloids (±)‐Budmunchiamine A – C

The syntheses of four macrocyclic spermine alkaloids, (±)‐budmunchiamine A – C ( 1a – c ) and (±)‐budmunchiamine L4 ( 1 ), were accomplished by Michael addition of spermine to the α,β‐unsaturated esters 3a – d , followed by cyclization of the resulting α,ω‐tetraamino esters 4a – d with triethoxyantimony; N‐methylation of the amino lactams 6a – c yielded the budmunchiamines A – C ( 1a – c ).     

4‐Substituted 2,3‐Dihydroisoxazoles as Masked Azomethine Ylides: Access to Pyrrole Derivatives by 1,5‐ and 1,7‐Dipolar Electrocyclizations of Enynyl Derivatives

The enynyl‐substituted 2,3‐dihydroisoxazoles (‘isoxazolines') 9 – 14 were prepared by highly (Z)‐selective Peterson olefination reaction from the corresponding carbaldehydes 6 – 8 . On short‐time thermolysis (280 – 406°/10 s) the TMS derivatives 9 – 11 give rise to the annulated pyrrolines 18 – 20 , which, in some cases, suffer CH₄ elimination affording the pyrroles 15 – 17 . In contrast, thermolysis of the terminal alkyne derivatives 12 – 14 leads to the bicyclic compounds 21 – 23 . The reaction pathways are discussed on the basis of the formation of conjugated azomethine ylides as key intermediates, which either undergo a 1,5‐cyclization to 18 – 20 or a 1,7‐ring‐closure affording cycloallene intermediates of type V , which are further transformed into the azepino pyrroles 21 – 23 .     

Molecular engineering of liquid crystal polymers by living polymerization. II. Living cationic polymerization of 11-[(4-cyano-4′-biphenyl) oxy] undecanyl vinyl ether and the mesomorphic behavior of the resulting polymers

The synthesis and living cationic polymerization of 11-[(4-cyano-4′-biphenyl)oxy]-undecanyl vinyl ether ( 6 – 11 ) are described. The mesomorphic phase behavior of poly( 6 – 11 ) with different degrees of polymerization was compared to that of 6 – 11 and of 11-[(4-cyano-4′-biphenyl) oxy] undecanyl ethyl ether ( 8 – 11 ) which is the model compound of the monomeric structural unit of poly( 6 – 11 ). 6 – 11 displays a monotropic S_A and a monotropic nematic mesophase while 8 – 11 an enantiotropic S_A mesophase. Poly( 6 – 11 ) with low degrees of polymerization exhibits an enantiotropic S_A mesophase. Poly( 6 – 8 ) with high degrees of polymerization displays an enantiotropic S_X (i. e., an unidentified smectic phase) and an enantiotropic S_C mesophase. These results demonstrate that the transformation of the nematic mesophase of the monomer into a smectic mesophase after polymerization, occurs at the level of monomeric structural unit.     

Synthesis and Characterization of Bis(2‐iminopyrrolyl) Iron(II) Complexes by N–H Bond Activation

The reactions of 2‐iminopyrroles 1 – 3 with Fe(PMe₃)₄ afforded the N–H activated bis(2‐iminopyrrolyl) iron(II) complexes 4 – 6 . The structures of compounds 4 – 6 were determined by single‐crystal X‐ray diffraction. The formation mechanism of complexes 4 – 6 was discussed.     

Synthesis and Characterization of New Thebaine Derivatives as Potential Opioid Agonists and Antagonists: 2‐[N‐(1H‐Tetrazol‐5‐yl)‐6,14‐endo‐etheno‐6,7,8,14‐tetrahydrothebaine‐7α‐yl]‐5‐phenyl‐1,3,4‐oxadiazoles

In this study, we report the synthesis a series of novel 2‐[N‐(1H‐tetrazol‐5‐yl)‐6,14‐endo‐etheno‐6,7,8,14‐tetrahydrothebaine‐7α‐yl]‐5‐phenyl‐1,3,4‐oxadiazole derivatives ( 7a – e ) which have potential opioid antagonist and agonist. The substitution reaction of 6,14‐endo‐ethenotetrahydrothebaine‐7α‐carbohydrazide with corresponding benzoyl chlorides gave diacylhydrazine compounds 4a – e in good yields. The treatment of compounds 4a – e with POCl₃ caused the conversion of side‐chain of compounds 5a – e into 1,3,4‐oxadiazole ring at C(7) position; thus, compounds 5a – e were obtained. Subsequently, cyanamides ( 6a – e ) were prepared from compounds 5a – e and then compounds 7a – e were synthesized by the azidation of 6a – e with NaN₃. The structures of the compounds were established on the basis of their IR, ¹H NMR, ¹³C APT, 2D‐NMR (COSY, NOESY, HMQC, HMBC) and high‐resolution mass spectral data.     

Condensed 1,2,4-Triazines I: Behaviour of Phenanthro[9,10-e]-1,2,4-triazine Derivatives Towards Alkylating and Reducing Agends,Grignard Reagents,and Amines

Alkylation of 3-hydroxy-phenanthro[9,10-e]1,2,4-triazine ( 1a ) yielded the N(2)-alkyl derivatives 2a – 2b ; alkylation of the 3-mercapto analogue 1b yielded the S-alkyl derivatives 1f – 1i . 1a – 1b reacted with alkyl and aralkylmagnesium halides to yield the corresponding 3-hydroxy-, and 3-mercapto-5-alkyl-(aralkyl)-phenanthro[9,10-e]2,3,4,5-tetrahydro-1,2,4-triazines 5a – 5f . Reduction of 1a yielded the hexahydrotriazine derivative 7 . Amination of 1c yielded the 3-amino derivatives 1j – 1o after prolonged heating.     

Synthesis of Novel 4‐Substituted Coumarins,Docking Studies,and DHODH Inhibitory Activity

Coumarins are the important class of naturally occurring heterocyclic compounds. Activities like antioxidant, antibacterial, anti‐inflammatory, and anticancer have been reported for coumarin derivatives. Present work details the synthesis of substituted coumarin‐4‐pyrrolones as well as coumarin‐4‐acetyl amino acids and their DHODH inhibitory activity, which is a dual target for malaria and cancer. Coumarin‐4‐acetic acids ( 2a – c ) were coupled with different methyl esters of α‐amino acids ( 3 ) giving rise to corresponding coumarin‐4‐acetyl amino acid methyl esters ( 4a – o ), which on hydrolysis under basic condition underwent cyclization forming substituted dihydropyrrole‐2‐ones ( 5a – i ), dihydroindolizine‐3‐ones ( 5j – l ), and dihydropyrrolizin‐3‐one ( 5m – o ). Acidic hydrolysis of the compounds ( 4a – o ) yielded corresponding coumarin‐4‐acetyl amino acids ( 6a – f ). The docking study was performed with the protein 4IGH (obtained from PDB) using Surflex–Dock module. The newly synthesized compounds were tested for DHODH inhibitory activity using Brequinar as the standard. Compound 6b showed remarkable inhibition compared with the standard, and the other compounds with terminal COOH showed moderate inhibition.     

Notiz zur Synthese von Alkyl-, Cycloalkyl- und Aryl-3-aminophenylsulfonen

Syntheses of Some Alkyl, Cycloalkyl and Aryl 3-Aminophenyl Sulfones Syntheses of alkyl ( 1a – 1i, 1m ), cycloalkyl ( 1j, 1k ) and aryl ( 1l ) 3-aminophenyl sulfones were achieved by ethanolic Béchamp-reduction of the appropriate 3-nitrophenyl sulfones ( 3a – 3m ). The alkyl ( 3a – 3i ) and cycloalkyl ( 3j, 3k ) 3-nitrophenyl sulfones were prepared via nitration of their respective sulfones ( 2a – 2k ). Methyl (3-nitrophenyl) sulfone ( 3a ) was also prepared by condensation of 3-nitrobenzenesulfinic acid ( 4 ) with bromoacetic acid to 3-nitrophenylsulfonyl-acetic acid ( 5 ) followed by decarboxylation.     

β-Cleavage of Bis(homoallylic) Potassium Alkoxides. Preparation of 3-Hydroxypropyl and 4-Hydroxybutyl Propenyl Ketones from γ- and δ-Lactones. Synthesis of (±)-Rose oxide

Starting from γ- and δ-lactones 1 – 3 , a two-step preparation of 3-hydroxypropyl and 4- hydroxybutyl propenyl ketones 10 – 18 is described, involving as the key step the β-cleavage of the bis(homoallylic) potassium alkoxides 4a – 9a . The novel methodology is illustrated by a short synthesis of (±)-rose oxide( 20 ).     

Separation of Aminoglycosides by Normal- and Reversed-Phase TLC

JPC – Journal of Planar Chromatography – Modern TLC - The normal-phase (NP) and reversed-phase (RP) thin-layer chromatographic separations of aminoglycosides (streptomycin, kanamycin,...     

Pteridines,Part CXI,Pteridine‐Based Photoaffinity Probes for Nitric Oxide Synthase and Aromatic Amino Acid Hydroxylases

Various 6‐substituted pteridines and 5,6,7,8‐tetrahydropterins carrying photolabile functions at the side chain (see 7 , 20 – 22 , 34 – 36 , 38 , and 39 ) as well as at the 5‐position (see 27 – 29 ) were synthesized from pterin and from 6‐phenylpterin ( 1 ) and 6‐(hydroxymethyl)pterin ( 10 ). Attachment of the photoaffinity labels via ester bonds required a special protecting‐group strategy based upon acid‐labile (see 30 – 33 ) and β‐eliminating blocking groups (see 17 – 19 ). The 6‐(4‐azidophenyl)pterin ( 7 ) was obtained from 6‐phenylpterin ( 1 ) via intermediates 2 and 4 – 6 , due to the low solubility of simple pterins in general. The pteridine derivatives 21 , 22 , 25 , 26 , 28 , 29 , 32 , 33 , 35 , 36 , 38 , and 39 were screened as inhibitors of neuronal (type I) NO synthase (see Table) from porcine cerebellum, of which 22 , 35 , 36 , and 38 showed interesting inhibitory activity with similar potency and effectiveness.     

Enantiomeric Thin-Layer Chromatographic Assay of Escitalopram in Presence of “In-Process Impurities”

JPC – Journal of Planar Chromatography – Modern TLC - A simple, rapid and precise thin-layer chromatographic (TLC) method for analysis of escitalopram oxalate (ESC-OX) (S-enantiomer) in...     

Application of TLC and OPLC in the Determination of Pigments from Natural Products

JPC – Journal of Planar Chromatography – Modern TLC - Planar chromatographic methods thin-layer chromatography (TLC) and over-pressure thin-layer chromatography (OPLC) have been...     

The unusual fragmentation of long‐chain feruloyl esters under negative ion electrospray conditions

Long‐chain ferulic acid esters, such as eicosyl ferulate ( 1 ), show a complex and analytically valuable fragmentation behavior under negative ion electrospay collision‐induced dissociation ((?)‐ESI‐CID) mass spectrometry, as studied by use of a high‐resolution (Orbitrap) mass spectrometer. In a strong contrast to the very simple fragmentation of the [M + H]⁺ ion, which is discussed briefly, the deprotonated molecule, [M – H]^?, exhibits a rich secondary fragmentation chemistry. It first loses a methyl radical (MS²) and the ortho‐quinoid [M – H – Me]^‐? radical anion thus formed then dissociates by loss of an extended series of neutral radicals, C_nH_2n + 1^? (n = 0–16) from the long alkyl chain, in competition with the expulsion of CO and CO₂ (MS³). The further fragmentation (MS⁴) of the [M – H – Me – C₃H₇]^? ion, discussed as an example, and the highly specific losses of alkyl radicals from the [M – H – Me – CO]^‐? and [M – H – Me – CO₂]^‐? ions provide some mechanistic and structural insights.     

Stability-Indicating Methods for the Determination of Luliconazole by TLC and HPTLC-Densitometry in Bulk Powder and Cream Dosage Form

JPC – Journal of Planar Chromatography – Modern TLC - Rapid and sensitive thin-layer chromatography (TLC) and high-performance thin-layer chromatography (HPTLC)—densitometry...