N-Ethynylation of Anilides Decreases the Double-Bond Character of Amide Bond while Retaining trans-Conformation and Planarity

Activated amide bonds have been attracting intense attention; however, most of the studied moieties have twisted amide character. To add a new strategy to activate amide bonds while maintaining its planarity, we envisioned the introduction of an alkynyl group on the amide nitrogen to disrupt amide resonance by nN→C_sp conjugation. In this context, the conformations and properties of N-ethynyl-substituted aromatic amides were investigated by DFT calculations, crystallography, and NMR spectroscopic analysis. In contrast to the cis conformational preference of N-ethyl- and vinyl-substituted acetanilides, N-ethynyl-substituted acetanilide favors the trans conformation in the crystal and in solution. It also has a decreased double bond character of the C(O)−N bond, without twisting of the amide. N-Ethynyl-substituted acetanilides undergo selective C(O)−N bond or N−C(sp) bond cleavage reactions and have potential applications as activated amides for coupling reactions or easily cleavable tethers.     

Acid‐Promoted Chemoselective Introduction of Amide Functionality onto Aromatic Compounds Mediated by an Isocyanate Cation Generated from Carbamate

Carbamates have been used as precursors of isocyanates, but heating in the presence of strong acids is required because cleavage of the C? O bond in carbamates is energy‐demanding even in acid media. Direct amidation of aromatic compounds by isocyanate cations generated at room temperature from carbamoyl salicylates in trifluoromethanesulfonic acid (TfOH) was examined. Carbamates with ortho‐salicylate as an ether group (carbamoyl salicylates) showed dramatically accelerated O? C bond dissociation in TfOH, which resulted in facile generation of the isocyanate cation. These chemoselective intermolecular aromatic amidation reactions proceeded even at room temperature and showed good compatibility with other electrophilic functionalities and high discrimination between N‐monosubstituted carbamate and N,N‐disubstituted carbamate. The reaction rates of secondary and tertiary amide formation were markedly different, and this difference was utilized to achieve successive (tandem) amidation reactions of molecules with an N‐monosubstituted carbamate and an N,N‐disubstituted carbamate with two kinds of aromatic compounds.     

2,2,5,5,8,8‐Hexa­methyl‐2,3,5,6,7,8‐hexa­hydro­imidazo­[1,2‐a]­pyrazine‐3,6‐dione,a bicyclic product of α‐amino­isobutyric acid condensation

The title compound, C₁₂H₁₉N₃O₂, is an unusual product of silica‐catalyzed intermolecular condensation of α‐amino­isobutyric acid. The mol­ecule has three types of C—N bonds: a double bond, a cis‐amide bond and single bonds, two of which are typical and two having intermediate lengths due to π‐electron delocalization between C=N and C=O groups. The cis‐amide moieties interact to form dimers via hydrogen bonds which stack in parallel layers.     

Key Role of Intramolecular Metal Chelation and Hydrogen Bonding in the Cobalt‐Mediated Radical Polymerization of N‐Vinyl Amides

This work reveals the preponderance of an intramolecular metal chelation phenomenon in a controlled radical polymerization system involving the reversible trapping of the radical chains by a cobalt complex bis(acetylacetonato)cobalt(II). The cobalt‐mediated radical polymerization (CMRP) of a series of N‐vinyl amides was considered with the aim of studying the effect of the cobalt chelation by the amide moiety of the last monomer unit of the chain. The latter reinforces the cobalt? polymer bond in the order N‐vinylpyrrolidone<N‐vinyl caprolactam<N‐methyl‐N‐vinyl acetamide, and is responsible for the optimal control of the polymerizations observed for the last two monomers. Such a double linkage between the controlling agent and the polymer, through a covalent bond and a dative bond, is unique in the field of controlled radical polymerization and represents a powerful opportunity to fine tune the equilibrium between latent and free radicals. Possible hydrogen bond formation is also taken into account in the case of N‐vinyl acetamide and N‐vinyl formamide. These results are essential for understanding the factors influencing Co? C bond strength in general, and the CMRP mechanism in particular, but also for developing a powerful platform for the synthesis of new precision poly(N‐vinyl amide) materials, which are an important class of polymers that sustain numerous applications today.     

Synthesis and characterization of model compounds for carbazole-substituted N-acylated linear polyethylenimine (PEI). Synthesis and 1H-NMR spectra of N-acylated diethylamine and N,N′-dimethyl-1,2-ethanediamine containing 9-carbazolylacetyl, (R,S)- or (R)-2-(9-carbazolyl)propanoyl groups

The synthesis of N,N-diethyl-9-carbazolylacetamide ( 6 ), (R,S)- and (R)-N,N-diethyl-2-(9-carbazolyl)propanamide ( 7 ), N,N′-dimethyl-N,N′-di-(9-carbazolylacetyl)-1,2-ethanediamine ( 11 ), and (R)-N,N′-dimethyl-N,N′-di[2-(9-carbazolyl)propanoyl]-1,2-ethanediamine ( 13 ) is reported. The racemic compound, (R,S)-2-(9-carbazolyl)propanoic acid ( 2 ), was resolved by partial crystallization of the diastereomeric salts formed between 2 and (+)-α-methylbenzylamine. The ¹H-NMR spectra of 6 and 7 showed magnetic nonequivalence of the chemically equivalent protons of the methyl and methylene groups in 6 and 7 due to partial double bond character of the amide bond. The upfield resonances corresponding to the two sets of methyl and methylene protons were assigned by the aromatic solvent-induced shift (ASIS) method to the protons anti to the carbonyl oxygen in the conformation of amide bond in 6 and 7 . The ¹H-NMR spectra of 11 and (R)- 13 were used to determine the population of anti-anti, anti-syn (syn-anti) and syn-syn conformers in the structures of these dimer model compounds; the relative conformer populations were 0.45:0.47:0.08 and 0.28±0.02:0.29±0.01:0.43±0.01 in 11 and (R)- 13 .     

Preparation of 3-Oxo- and 3-Ethylideneazetidine Derivatives

The preparation of 3-azetidinones with different N-substituents and their transformation to 3-ethylideneazetidines has been studied in relation with a projected synthesis of 3-ethylideneazetidine-2-carboxylic acid (= polyoximic acid; 1 ). The stable crystalline 3-azetidinone hydrochloride ( 18 ), obtained by hydrogenolysis of the known 1-(diphenylmethyl)-3-azetidenone ( 4 ), is described for the first time, From this key intermediate, 3-oxoazetidine-derived amides, exemplified by benzamide 12 ,urethanes (e.g. 17 ), and ureas (e.g. 20 ) can be prepared in good yield (Scheme 3). The olefination of 3-azetidinones with alkylidene(triphenyl)phosphoranes is a perparatively useful process only for derivatives with a pyramidal N-atom, e.g. the diphenylmethyl derivative 4 , and not for the amide 12 or the urethane 17 (Scheme 4). 3-Alkylidene-azetidines with an amide N-atom should, therefore, be prepared by exchange of the N-substituent after the introduction of the double bond.     

A pipecolic acid (Pip)‐containing dipeptide,Boc‐d‐Ala‐l‐Pip‐NHiPr

The title dipeptide, 1‐(tert‐butoxy­carbonyl‐d ‐alanyl)‐N‐iso­propyl‐l ‐pipecol­amide or Boc‐d ‐Ala‐l ‐Pip‐NHⁱPr (H‐Pip‐OH is pipecolic acid or piperidine‐2‐carboxylic acid), C₁₇H₃₁N₃­O₄, with a d –l heterochiral sequence, adopts a type II′β‐­turn conformation, with all‐trans amide functions, where the C‐terminal amide NH group interacts with the Boc carbonyl O atom to form a classical i+3 i intramolecular hydrogen bond. The C^α substituent takes an axial position [H^α (Pip) equatorial] and the trans pipecolamide function is nearly planar.     

Acet­amidoxime

The oxime of acet­amide, viz. N‐hydroxy­ethanimid­amide, C₂H₆N₂O, has a complex hydrogen‐bonding arrangement in its crystal structure, featuring one strong O—H⋯N hydrogen bond together with weaker hydrogen bonding involving the amide groups. Conjugation effects lead to atypical distances and angles.     

Conformational effects in cyclic imino acids—I: The NMR spectra and conformations of l-azetidine-2-carboxylic acid and its N-acetyl derivative

The complete analysis of the PMR spectrum of azetidine-2-carboxylic acid is reported and conclusions made regarding the conformation of the molecule in aqueous solution. the effect of N-acetylation on chemical shifts, coupling constants and hence conformation is investigated, and the geometric isomer ratio and energy barrier to rotation about the amide bond determined.     

New synthetic route to alternating copoly(aromatic ester–aliphatic amide)s

The preparation of three novel alternating copoly(aromatic ester–aliphatic amide)s containing the same ordered amide–amide–ester–ester (AAEE), the same para-disubstituted phenyl, and the different long methylene chain structure were described. 1,1′-(Adipoyl)bisbenzotriazole (AdBBT), 1,1′-(suberoyl)bisbenzotriazole (SuBBT), and 1,1′-(sebacoyl)bisbenzotriazole (SeBBT) were synthesized. These diacylbenzotriazoles were preferred to aminoethanol at the amino group because of the selective N-acylation of active acylamide of benzotriazole in excellent yield at room temperature to give diol monomers such as N,N′-bis(2-hydroxyethyl)adipic amide (HEAdA), N,N′-Bis(2-hydroxyethyl)subaric amide (HESuA), and N,N′-bis(2-hydroxyethyl)sebacic amide (HESeA). Polycondensation of 1,1′-(teraphthaloyl)bisbenzotrizole (tPBT) with HEAdA, HESuA, and HESeA gave the corresponding alternating copoly(aromatic ester–aliphatic amide)s: P(tPE–AdA), P(tPE–SuA), and P(tPE–SeA), respectively. The alternating copoly(aromatic ester–aliphatic amide)s were characterized by ¹H-NMR spectra. The resulting polymers have two different chain units; one is chain unit of poly(ethylene terephthalate) and the other is a chain unit of polyamide-2,6, polyamide-2,8, and polyamide-2,10; both are linked via a C? N bond.     

The deoxydative substitution reactions of nicotinamide and nicotinic acid N-oxides by 1-adamantanethiol in acetic anhydride

The reaction of nicotinamide N-oxide with 1-adamantanethiol in acetic anhydride yielded a mixture of 2-and 6-(1-adamantylthio)nicotinamides (49%, in the ratio of 24:1) and 2-, 5-, and 6-(1-adamantylthio)nicotino-nitriles (18%, in the ratio of 79:1:20). From a reaction of nicotinic acid N-oxide with 1-adamantanethiol, there was isolated 2-(1-adamantylthio)nicotinic acid as the only sulfide in 23% yield. Carbon? sulfur bond cleavage took place when 2-(1-adamantylthio)nicotinic acid, or the corresponding amide or nitrile, were boiled with concentrated hydrochloric acid to furnish 2-mercaptonicotinic acid and 1-chloroadamantane, quantitatively. The reaction of nicotinamide N-oxide alone in acetic anhydride at 135° formed N-acetyl-2-hydroxynicotinamide (61%), 2-hydroxynicotinonitrile (0.5%) and N,N-diacetyl-2-acetoxynicotinamide (0.8%).     

Structure dependence in the solvolysis kinetics of amino acid esters

To better understand acyl transfer reactions of oligopeptides, seventeen N-acyl amino acid esters were solvolyzed in mildly basic methanol-d₄. All show pseudo-first-order kinetics by ¹H NMR. The rate constant varies up to 400-fold with the identity of the amino acid and up to 6200-fold with the identity of the N-acyl group. The impact of the N-acyl group on the rate constant is discussed in terms of crowding, amide conformation, and amide CO bond character.     

Conformational isomerization of <Emphasis Type="Italic">N</Emphasis>-(naphthalen-1-yl)-<Emphasis Type="Italic">N</Emphasis>-(phenyl(quinolin-3-yl)methyl)amide derivatives

A series of N-(naphthalen-1-yl)-N-(phenyl(quinolin-3-yl)methyl)amide derivatives were designed and synthesized as anti-Mycobacterium tuberculosis drugs. NMR spectra showed that two conformational isomers of these compounds exist in solution, which is not due to cis-trans isomerization of amide bond. We proposed that the spatial interactions between three large aromatic groups caused the conformational isomerization, which was supported by molecular modeling and X-ray diffraction.     

NEW DERIVATIVES OF 4,5-BENZO-1,3,2-OXAZA (OR D1AZA)-PHOSPHOLANE FROM CONVENIENT CONDENSATION OF SUBSTITUTED UREA WITH TRIS(DIALKYLAMINO)PHOSPHINE

Abstract

The condensation of N-phenyl-N′-(2-hydroxylphenyl)urea or N-phenyl-N′-(2-aminophenyl)urea with tris(dia1kylamino)phosphine afforded derivatives of 4,5-benzo-1,3,2-oxaza (or diaza)-phospholane which formed intramolecular hydrogen bond. The cleavage of the amide bond to give N,N-dialky1-N′-phenylurea together with polymers of 1,3,2-benzodiazaphosphole was observed in the latter reaction.     

Base-catalyzed polymerization of acryloyl- and methacryloyl-α-amino acid amides

N-Acryloylglycinamide, N-methacryloylglycinamide, N-acryloyl-DL - and L -alaninamide, and N-methacryloyl-DL - and -L -alaninamide were polymerized by basic catalysts. Polymers with low viscosities were obtained. Automatic amino acid analyses of the hydrolyzates of these polymers indicated that a hydrogen transfer from the terminal amide group took place along with vinyl polymerization. Hydrogen transfer from the secondary amide group was also observed. The ratio of the hydrogen transfer and the vinyl polymerizations was determined by results of automatic amino acid analyses.     

Structures of Highly Twisted Amides Relevant to Amide N−C Cross‐Coupling: Evidence for Ground‐State Amide Destabilization

Herein, we show that acyclic amides that have recently enabled a series of elusive transition‐metal‐catalyzed N?C activation/cross‐coupling reactions are highly twisted around the N?C(O) axis by a new destabilization mechanism of the amide bond. A unique effect of the N‐glutarimide substituent, leading to uniformly high twist (ca. 90°) irrespective of the steric effect at the carbon side of the amide bond has been found. This represents the first example of a twisted amide that does not bear significant steric hindrance at the α‐carbon atom. The ¹⁵N NMR data show linear correlations between electron density at nitrogen and amide bond twist. This study strongly supports the concept of amide bond ground‐state twist as a blueprint for activation of amides toward N?C bond cleavage. The new mechanism offers considerable opportunities for organic synthesis and biological processes involving non‐planar amide bonds.     

Directed H-bonding inhibition in molecular recognition: an NMR case study of the H-bonding of a dicarboxylic acid with a new mixed diamide receptor having one adjacent pyridine-N-oxide

The inhibition of hydrogen bond formation in the recognition of adipic acid by a new diamide receptor 1 having a pyridine-N-oxide and a simple pyridine ring adjacent to the amide moieties is observed. NMR studies show binding by the pyridine amide group in 1, which demonstrates the discrimination in hydrogen bonding between the carboxyls and an amide adjacent to pyridine versus another adjacent to the pyridine N-oxide. This specific inhibition of hydrogen bonding to a carboxyl group by the two different amides in 1 is corroborated by the NMR binding studies of 1 with propionic acid.     

Syntheses of some hexacarboxylic acid derivatives of hexaazatriphenylene

Synthetic methods and product characterizations for the conversions of 1,4,5,8,9,12-hexaazatriphenylene-hexacarboxylic acid to the corresponding triester triacid, triamic acid, triimide, triester triacid chloride, trimethyl triethyl hexaester, trimethyl ester tri(N,N-dimethyrjamide, hexaamide, tri(N,N,-dimethyr)amide triacid, tri(N,N-dimethyl)amide triacid chloride, and trisphthalhydrazide derivatives are described.     

Electrophilicity Scale of Activated Amides: 17O NMR and 15N NMR Chemical Shifts of Acyclic Twisted Amides in N−C(O) Cross-Coupling

The structure and properties of amides are of tremendous interest in organic synthesis and biochemistry. Traditional amides are planar and the carbonyl group non-electrophilic due to n_N→π*_C=O conjugation. In this study, we report electrophilicity scale by exploiting ¹⁷O NMR and ¹⁵N NMR chemical shifts of acyclic twisted and destabilized acyclic amides that have recently received major attention as precursors in N-C(O) cross-coupling by selective oxidative addition as well as precursors in electrophilic activation of N-C(O) bonds. Most crucially, we demonstrate that acyclic twisted amides feature electrophilicity of the carbonyl group that ranges between that of acid anhydrides and acid chlorides. Furthermore, a wide range of electrophilic amides is possible with gradually varying carbonyl electrophilicity by steric and electronic tuning of amide bond properties. Overall, the study quantifies for the first time that steric and electronic destabilization of the amide bond in common acyclic amides renders the amide bond as electrophilic as acid anhydrides and chlorides. These findings should have major implications on the fundamental properties of amide bonds.     

Hydrogen bonding between carboxylic acids and amide-based macrocycles in their host–guest complexes

For 12- and 13-membered macrocycles in which two amide linkages are integrated in the macrocyclic ring systems, the formation of 1:1 host–guest complexes with acetic and benzoic acids has been confirmed by NMR titrations. The complex formation occurs with the formation constants of 8–27 M^? 1, under competition with the dimerisation of acid molecules. Benzoic acid tends to form more stable complexes than acetic acid. The binding force is due to a pair of hydrogen bonds, O_carboxyl–H…O = C_amide and C = O_carboxyl…H–N_amide, between the carboxyl group of a guest molecule and the amide group of a host molecule. The former bond is stronger than the latter, and defines the stability of the complexes. The formation of the pair of hydrogen bonds is accompanied by the conformational conversion of the amide group from the trans-form to the cis-form. The influence of such a conversion on the internal molecular motion is observed as a slight broadening of signal width.

For 12- and 13-membered macrocycles in which two amide linkages are integrated in the macrocyclic ring systems, the formation of 1:1 host–guest complexes with acetic and benzoic acids has been confirmed by NMR titrations. The binding force for the complex formation is due to a pair of hydrogen bonds, O_carboxyl–H…O = C_amide and C = O_carboxyl…H–N_amide. The former bond is stronger than the latter and dominates the hydrogen-bond formation. The formation of the pair of hydrogen bonds is accompanied by the conformational conversion of the amide group from the stable trans-form to the less stable cis-form.