Synthesis of bis-3-alkyl-5-arylhydantoins and bis-3-alkyl-5-arylthiohydantoins separated by two and four carbon atoms

Synthesis of 1,2- and 1,4-bis-thiohydantoins and hydantoins employing ethylenediamine and 1,4-diaminobutane as spacers is described. Compounds containing a two carbon bridge were synthesized by alkylation of ethylenediamine with two equivalents of N-t-butyl-α-(p-toluenesulfonyloxy)phenylacetamide 3 . The phenyl isothiocyanate adduct of 3 cyclized in refluxing toluene to form 1a . Other isothiocyanate or isocyanate adducts derived from alkylation product 4 required hydrolysis to induce cyclization. Compounds 1b-1f were obtained in this way. Compounds with a four carbon bridge were obtained by reaction of two equivalents of methyl α-bromophenyl acetate and 1,4-diaminobutane to produce N,N'-bis-[(α-phenyl-α-methoxycarbonyl)methyl]butylenediamine 6 . The isothiocyanate or isocyanate adducts from 6 cyclized, without hydrolysis, to form compounds 2a-2e .     

Promoting effects of urethane derivatives of phenols on the ring‐opening polymerization of 1,3‐benzoxazines

For the purpose of reducing the induction period of the ring‐opening polymerization of N‐methyl‐1,3‐benzoxazines, several urethanes were examined as promoters. The examined promoters 3a – d were the adducts of resorcinol and phenyl isocyanate, that of bisphenol A and phenyl isocyanate, that of resorcinol and butyl isocyanate, and that of 1,3‐propanediol and phenyl isocyanate, respectively. The aromatic urethanes 3a and 3b , which were adducts of the phenolic compounds and phenyl isocyanate, exhibited significant promoting effects. © 2011 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem, 2011     

Evaluation and Comparison of a 3,5‐Dimethylphenyl Isocyanate Teicoplanin with Phenyl Isocyanate Teicoplanin Chiral Stationary Phase Using RP‐HPLC

HPLC enantiomeric separations of 8 α‐amino acids were achieved using two self‐made chiral stationary phases (CSP)–phenyl isocyanate teicoplanin (Phe‐TE) and 3,5‐dimethylphenyl isocyanate teicoplanin (DMP‐TE), using reversed phase mobile phases. The Phe‐TE or the DMP‐TE CSP was prepared from the TE using derivative agents, phenyl isocyanate or 3,5‐dimethylphenyl isocyanate, respectively. The chromatographic results were given as the retention, selectivity, resolution factor and the enantioselective free energy difference corresponding to the separation of the two enantiomers. The effect of pH, organic modifier type and amount were discussed, and the stereoselectivities for two TE‐based CSPs were compared. The chiral selectivity factor for six α‐amino acids on DMP‐TE is somewhat bigger than that on Phe‐TE CSP under reversed phase (RP) mode. Comparison of the enantiomeric separations using self‐made Phe‐TE and DMP‐TE was conducted to gain a better understanding of the chiral recognition mechanism of the macrocyclic glycopeptide CSP.     

Multinuclear NMR studies and ab initio structure calculations of hindered phencyclone diels‐alder adducts from symmetrical cyclic dienophiles: Cyclohexene,vinylene carbonate,vinylene trithiocarbonate and two N‐aryl maleimides

A series of hindered Diels‐Alder adducts have been prepared from phencyclone, 1 , with various unusual symmetrical cyclic dienophiles, including cyclohexene, 2a ; vinylene carbonate, 2b ; vinylene trithiocarbonate, 2c ; and the N‐aryl maleimides: N‐(4‐dimethylamino‐3,5‐dinitrophenyl)maleimide (“Tuppy's maleimide”), 2d ; and N‐[3,5‐bis(trifluoromethyl)phenyl]maleimide, 2e . The highly hindered adducts, 3a‐e , respectively, were extensively characterized by one‐ and two‐dimensional NMR methods, observing proton, carbon‐13 and fluorine‐19. High resolution COSY45 spectra permitted rigorous proton NMR assignments. The 2D heteronuclear C‐H chemical shift correlation spectra (HETCOR, XHCORR) were obtained for adducts 3a‐d , allowing specific assignments for protonated carbons. Corrections to earlier proton NMR assignments for the vinylene carbonate adduct are given; results of the gated decoupling ¹³C NMR experiment for this adduct supported endo adduct stereochemistry. Relative proton chemical shifts for bridgehead phenyls of adduct 3c appeared anomalous relative to other adducts, suggesting possible special anisotropic interactions (with endocyclic sulfur or other anisotropic groups in the product) due to the unusual calculated orientation of the phenyls. The unsubstituted bridgehead phenyls in all adducts were shown to exhibit slow exchange limit (SEL) ¹H and ¹³C spectra on the NMR timescales at ambient temperatures (7 tesla) showing slow rotations about the C(sp³)‐C(aryl sp²) bonds. The rapid rotation of the N‐aryl rings of the maleimide adducts was indicated by fast exchange limit spectra, suggesting that ortho substitution of the N‐aryl ring may be necessary to slow this rotation to the SEL regime. Ab initio geometry optimizations at the Hartree‐Fock level were carried out for each adduct, with the 6‐31G* basis sets. Appreciable geometry differences were seen in calculated structures, and significant NMR chemical shift differences were experimentally observed, depending on the nature of the groups attached to the (Z)‐HC=CH moiety of the dienophiles.     

Synthesis and properties of aromatic secondary amine-blocked isocyanates

N-Methylaniline-, diphenylamine-, and N-phenylnaphthylamine-blocked toluene diisocyanates (TDI) were prepared and characterized by IR, NMR spectroscopy, and nitrogen content analyses. The structure–property relationship of these adducts was established by reacting with hydroxyl-terminated polybutadiene (HTPB). The cure rate of the adduct increases from the N-phenylnaphthylamine- to diphenylamine- and to N-methylaniline-blocked TDI adduct. Simultaneous TGA/DTA results also confirm this trend, and the thermal stability of the adduct decreases in the following order: N-phenylnaphthylamine–TDI > diphenylamine–TDI > N-methylaniline–TDI. The gas chromatogram of the amine-blocked isocyanate confirms that the thermolysis products are the blocking agent and isocyanate. The solubilities of the adducts were carried out in polyether, polyester, and hydrocarbon polyols, and it was found that the N-methylaniline–TDI adduct shows higher solubility than the rest and also found that the polyester polyol shows higher solvating power against the adducts than the polyether and hydrocarbon polyols. © 1999 John Wiley & Sons, Inc. J Polym Sci A: Polym Chem 37: 1815–1821, 1999     

Identification of modification sites on human serum albumin and human hemoglobin adducts with houttuynin using liquid chromatography coupled with mass spectrometry

Houttuynin, a β‐keto aldehyde compound, is the major active ingredient in herba houttuyniae injection. The injection was once used as an anti‐inflammatory drug associated with occasional serious hypersensitivity reactions in the clinic, which were proposed to be related to the formation of protein adducts. N^α‐Boc‐lysine, FEEM and IVTNTT were used as model amino acids or peptides containing one nucleophilic residue to investigate adduct types by liquid chromatography coupled with ion trap mass spectrometry (LC/MSⁿ) and high‐resolution quadrupole time‐of‐flight mass spectrometry (Q‐TOF MS). These adducts were respectively characterized as Schiff bases formed by 1:1 reaction of houttuynin with lysine or N‐terminal residue and pyridinium adducts by 2:1 reaction. LC/MSⁿ analysis of trypsin digests of HSA/Hb incubations with houttuynin revealed that houttuynin‐modified HSA adducts were formed mainly at N‐terminal amino acid and lysine residues, specifically at Lys‐212, Lys‐414 and Lys‐525 for Schiff base adducts, and at Lys‐414 and Lys‐432 for pyridinium adducts, and houttuynin adducted more readily with N‐terminal valine of the α‐ and β‐chains in Hb and lysine amine (Lys‐62) of the β‐chain for Schiff base adducts. The results showed the direct modification of houttuynin to HSA/Hb in vitro, which was speculated to be responsible for the adverse reactions induced by houttuyniae injection. Copyright © 2012 John Wiley & Sons, Ltd.     

Adamantanes as spherical nanosondes in adducts with a chiral dirhodium complex-discriminating enantiomers and probing spatial proximities

Three different kinds of substituted chiral adamantane molecules—adamantanones, dioxolanoadamantanes and dithiolano—adamantanes—were studied in the dirhodium experiment (NMR measurement with 1:1 molar mixtures with Rh^(II)₂[(R)‐(+)‐MTPA]₄ in CDCl₃). Their different behavior in adduct formation is described, and the possibility of determining enantiomeric purities and absolute configurations is explored. Detailed inspection of one‐ and two‐dimensional NMR experiments allowed for an interpretation of steric and electronic intra‐adduct interaction showing that the phenyl groups of Rh* tend to enwrap the bound adamantane ligand so that through‐space effects over a range of 6–7 Å away from the binding rhodium atom can be observed. Even slight differences in the relative orientation of phenyl groups can be monitored when comparing diastereomeric adducts via NMR signal dispersion. Copyright © 2011 John Wiley & Sons, Ltd.     

Preparation of 5,5′‐pyrilidene and 5,5′‐quinolidene bis‐barbituric acid derivatives

NMR reaction following experiments were used to find optimal conditions for the barbituric acid double addition to aromatic and heteroaromatic carboxaldehydes. It was established that aromatic aldehydes with electron‐donating substituents such as hydroxy, methoxy, and dimethylamino produce only the single addition barbituric acid adduct (barbituric acid benzylidenes). If these electron‐donating substituents are transformed into electron‐withdrawing substituents by virtue of protonation (NMe₂ to NHMe₂⁺) then the double barbituric acid adduct becomes the sole product of the reaction. This is also true regardless of the reaction media if strong electron‐withdrawing substituents (such as a nitro group) are present. Considering that the reactive species for nitrogen containing aromatic heterocycles are actually the conjugated acids (electron deficient molecule) only the double barbituric acid adducts are isolated. All synthetic procedures presented are applicable to multi‐gram scale preparations of double barbituric acid adducts.     

Adducts of nitrogenous ligands with rhodium(II) tetracarboxylates and tetraformamidinate: NMR spectroscopy and density functional theory calculations

Complexation of tetrakis(μ₂‐N,N'‐diphenylformamidinato‐N,N')‐di‐rhodium(II) with ligands containing nitrile, isonitrile, amine, hydroxyl, sulfhydryl, isocyanate, and isothiocyanate functional groups has been studied in liquid and solid phases using ¹H, ¹³C and ¹⁵N NMR, ¹³C and ¹⁵N cross polarisation–magic angle spinning NMR, and absorption spectroscopy in the visible range. The complexation was monitored using various NMR physicochemical parameters, such as chemical shifts, longitudinal relaxation times T₁, and NOE enhancements. Rhodium(II) tetraformamidinate selectively bonded only unbranched amine (propan‐1‐amine), pentanenitrile, and (1‐isocyanoethyl)benzene. No complexation occurred in the case of ligands having hydroxyl, sulfhydryl, isocyanate, and isothiocyanate functional groups, and more expanded amine molecules such as butan‐2‐amine and 1‐azabicyclo[2.2.2]octane. Such features were opposite to those observed in rhodium(II) tetracarboxylates, forming adducts with all kind of ligands. Special attention was focused on the analysis of Δδ parameters, defined as a chemical shift difference between signal in adduct and corresponding signal in free ligand. In the case of ¹H NMR, Δδ values were either negative in adducts of rhodium(II) tetraformamidinate or positive in adducts of rhodium(II) tetracarboxylates. Experimental findings were supported by density functional theory molecular modelling and gauge independent atomic orbitals chemical shift calculations. The calculation of chemical shifts combined with scaling procedure allowed to reproduce qualitatively Δδ parameters. Copyright © 2013 John Wiley & Sons, Ltd.     

Charge‐derivatized amino acids facilitate model studies on protein side‐chain modifications by matrix‐assisted laser desorption/ionization time‐of‐flight mass spectrometry

The α‐amino groups of histidine and lysine were derivatized with p‐carboxylbenzyltriphenylphosphonium to form the pseudo dipeptides, PHis and PLys, which can be sensitively detected by matrix‐assisted laser desorption/ionization time‐of‐flight mass spectrometry (MALDI‐TOFMS) due to the fixed positive charge of the phosphonium group. Detection limits of PHis and PLys by MALDI‐TOFMS were both 30 fmol with a signal‐to‐noise ratio of 5:1. These pseudo dipeptides were excellent surrogates for His‐ or Lys‐containing peptides in model reactions mimicking proteins with reactive electrophiles, prominently those generated by peroxidation of polyunsaturated fatty acids including 4‐hydroxy‐2(E)‐nonenal (HNE), 4‐oxo‐2(E)‐nonenal (ONE), 2(E)‐octenal, and 2(E)‐heptenal. An air‐saturated solution of linoleic acid (d₀:d₅ = 1:1) was incubated in the presence of Fe(II) and ascorbate with these two pseudo dipeptides, and the reaction products were characterized by MALDI‐TOFMS and liquid chromatography/electrospray ionization mass spectrometry (LC/ESI‐MS). By using PHis and PLys, the previously reported ONE‐derived His‐furan adduct was detected along with evidence for a cyclic α,β‐unsaturated ketone. A dimer formed from ONE was found to react with PHis through Michael addition. Alkenals were found to form two novel adducts with PLys. 2(E)‐Octenoic acid–His Michael adduct and N^ε‐pentanoyllysine were identified as potential protein side‐chain adducts modified by products of linoleic acid peroxidation. In addition, when PHis or PLys and AcHis or BocLys were exposed to the linoleic acid peroxidation, an epoxy‐keto‐ocatadecenoic acid mediated His–His cross‐link was detected, along with the observation of a His–ONE/9,12‐dioxo‐10‐dodecenoic acid–Lys derived pyrrole cross‐link. Copyright © 2009 John Wiley & Sons, Ltd.     

Synthesis and characterization of chiral poly(alkyl isocyanates) by coordination polymerization using a chiral half‐titanocene complex

A new chiral half‐titanocene complex, [CpTiCl₂(O‐(S)?2‐Bu)], is synthesized and characterized by ¹H and ¹³C NMR spectroscopy. This complex is employed for the coordination polymerization of n‐butyl and n‐hexyl‐ isocyanate leading to chiral polymers, as revealed by their CD spectra. Only the left‐handed helix is produced, due to the chiral (S)?2‐butoxy group, which is bound to the polymer chain end. The polymerization of 3‐(triethoxysilyl)propyl isocyanate produces less soluble polymers. On the other hand, phenyl isocyanate reacts slowly with the complex leading quantitatively and selectively to triphenyl isocyanurate. 2‐Ethylhexyl isocyanate is slowly and selectively cyclotrimerized in the presence of the half‐titanocene complex. However, a statistical copolymer of 2‐ethylhexyl isocyanate and hexyl isocyanate is produced. The reaction of benzyl isocyanate with the complex leads to a mixture of low molecular weight polymer and cyclotrimer. The polymers are characterized using SEC, NMR, and CD spectroscopy and their thermal properties are investigated by TGA/DSC analysis. © 2015 Wiley Periodicals, Inc. J. Polym. Sci., Part A: Polym. Chem. 2015 , 53, 2141–2151     

One‐Pot Synthesis of 4‐(Alkylamino)‐1‐(arylsulfonyl)‐3‐benzoyl‐1,5‐ dihydro‐5‐hydroxy‐5‐phenyl‐2H‐pyrrol‐2‐ones via a Multicomponent Reaction

An effective route to novel 4‐(alkylamino)‐1‐(arylsulfonyl)‐3‐benzoyl‐1,5‐dihydro‐5‐hydroxy‐5‐phenyl‐2H‐pyrrol‐2‐ones 10 is described (Scheme 2). This involves the reaction of an enamine, derived from the addition of a primary amine 5 to 1,4‐diphenylbut‐2‐yne‐1,4‐dione, with an arenesulfonyl isocyanate 7 . Some of these pyrrolones 10 exhibit a dynamic NMR behavior in solution because of restricted rotation around the C? N bond resulting from conjugation of the side‐chain N‐atom with the adjacent α,β‐unsaturated ketone group, and two rotamers are in equilibrium with each other in solution ( 10 ? 11 ; Scheme 3). The structures of the highly functionalized compounds 10 were corroborated spectroscopically (IR, ¹H‐ and ¹³C‐NMR, and EI‐MS), by elemental analyses, and, in the case of 10a , by X‐ray crystallography. A plausible mechanism for the reaction is proposed (Scheme 4).     

Addition von Acetylendicarbonsäuredimethylester an Imidazole; Aminierung der Addukte: neue Synthesen von 3-(2-Imidazolyl)-2-pyridon-4,5-dicarbonsäureamiden und Pyrido[1,2-a]pyrazinen

The reaction between dimethyl acetylene dicarboxylate and 2-amino-1-methylimidazole affords dimethyl 2-amino-1-methyl-1,3-diazepine-5,6-dicarboxylate in low yield. This 1:1 – adduct was formed by addition of the acetylenic compound to the enamine double bond of the imidazole ring followed by ring enlargement. On the other hand, 2:1 – adducts to the imine bond are isolated in moderate yield when dimethyl acetylene dicarboxylate is treated with either 1-methyl-2-methylmercapto-imidazole or 1-methyl-2-methylmercapto-imidazoline. These adducts behave differently on heating with ethylamine: the adduct of the imidazole series cyclizes to the pyridone 15 with concomittant loss of one carboxamide group whereas that of the imidazoline series forms a pyrido[1,2-a]pyrazine derivative 20 , both in high yield. The possible reaction mechanisms are discussed. ¹³C–NMR.-spectroscopy and X-ray analysis were used in the determination of several structures.     

Reactivity of a Frustrated Lewis Pair and Small‐Molecule Activation by an Isolable Arduengo Carbene?B{3,5‐(CF3)2C6H3}3 Complex

Tris[3,5‐bis(trifluoromethyl)phenyl]borane reacts with the sterically demanding Arduengo carbenes 1,3‐di‐tert‐butylimidazolin‐2‐ylidene and 1,3‐bis(2,6‐diisopropylphenyl)imidazolin‐2‐ylidene to form isolable normal adducts. In the case of 1,3‐di‐tert‐butylimidazolin‐2‐ylidene, the adduct exhibits dynamic behaviour in solution and frustrated‐Lewis‐pair (FLP) reactivity. Fast cleavage of dihydrogen and THF, the C? H activation of phenylacetylene, and carbon dioxide fixation were achieved by using solutions of this adduct in benzene. This adduct is stable at room temperature in the absence of suitable substrates; however, thermal rearrangement into an abnormal carbene–borane adduct can be observed. In contrast, the 1,3‐bis(2,6‐diisopropylphenyl)imidazolin‐2‐ylidene adduct exhibits no evidence of FLP reactivity or of dissociation in solution. DFT calculations confirmed the experimental behaviour and stability of these carbene–borane adducts.     

Dynamic Covalent Chemistry: A Facile Room‐Temperature,Reversible, Diels–Alder Reaction between Anthracene Derivatives and N‐Phenyltriazolinedione

A series of readily accessible, dynamic Diels–Alder reactions that are reversible at room temperature have been developed between anthracene derivatives as dienes and N‐phenyl‐1,2,4‐triazoline‐3,5‐dione as the dienophile. The adducts formed undergo reversible component exchange to form dynamic libraries of equilibrating cycloadducts. Furthermore, reversible adduct formation allows temperature‐dependent modulation of the fluorescent properties of anthracene components; a feature of potential interest for the design of optodynamic polymeric materials by careful selection and manipulation of these simple dienes and dienophiles.     

Characterization of Adducts Formed in the Reactions of Methylglyoxal and Malonaldehyde with Lysine and Histidine Derivatives

Glycation of biopolymers by α‐oxoaldehydes such as methylglyoxal is believed to play a major role in the complex pathologies associated with diabetes and metabolic diseases. To design strategies that could interfere with the endogenous production of such aldehydes or promote their detoxification or, alternatively, to develop therapeutic procedures that could inhibit the deleterious effects of the oxoaldehydes at the cellular level, it is important to characterize the wide spectrum of reactions between these compounds and biomolecules, and gain insight into their mechanisms. In this study, we investigated the reactivity of endogenous α‐oxoaldehyde, methylglyoxal, and of malonaldehyde towards amino acid derivatives, and we identified new adducts with N^α‐acetyllysine and N^α‐acetylhistidine. In addition, we showed that a structurally analogous adduct is also formed with the model peptide N‐acetylglycyllysine O‐methyl ester. The characterized compounds were most likely derived from the addition of the appropriate nucleophilic center of the studied biomolecules to the C?C bond of the initially formed aldehyde conjugate. The resulted adducts contain an electrophilic β‐dicarbonyl moiety and could potentially be involved in the formation of DNA? protein or protein cross? links.     

N-p-toluenesulfonyl-2-oxazolidones Via the cycloaddition reaction of p-tolucnesulfonyl isocyanate and epoxides

The reaction of styrene oxide and phenyl glycidyl ether with p-toluenesulfonyl isocyanate, employing a hydrocarbon-soluble adduct of tributylphosphine oxide and lithium bromide as catalyst, results in excellent yields of the N-p-toluenesulfonyl-2-oxazoIidones. The 5-isomeric-2-oxazolidone is obtained from phenyl glycidyl ether, but in contrast to conventional isocyanates, the p-toluenesulfonyl isocyanate, upon reaction with styrene oxide, produces the 4-isomeric 2-oxazolidone as the major product. The effect of the N-sulfonyl group on the nmr spectra of 2-oxazolidones is discussed.     

The Reactivities of Iminoboranes with Carbenes: BN Isosteres of Carbene–Alkyne Adducts

The first examples of adducts of cyclic alkyl(amino) carbenes (CAAC) and N‐heterocyclic carbenes (NHCs) with iminoboranes have been synthesized and isolated at low temperature (?45 °C). The adducts show short B?N bonds and planarity at boron, mimicking the structures of the isoelectronic imine functionality. When di‐tert‐butyliminoborane was reacted with 1,3‐bis(isopropyl)imidazol‐2‐ylidene (IPr), the initially formed Lewis acid–base adduct quickly rearranged to form a new carbene substituted with an aminoborane at the 4‐position. Warming the iminoborane–CAAC adduct to room temperature resulted in an intramolecular cyclization to give a bicyclic 1,2‐azaborilidine compound.     

Development of a Simple Adjustable Zinc Acid/Base Hybrid Catalyst for C−C and C−O Bond‐Forming and C−C Bond‐Cleavage Reactions

A newly designed zinc Lewis acid/base hybrid catalyst was developed. By adjusting the Lewis acidity of the zinc center, aldol‐type additions of 2‐picolylamine Schiff base to aldehydes proceeded smoothly to afford syn‐aldol adduct equivalents, trans‐N,O‐acetal adducts, in high yields with high selectivities. NMR experiments, including microchanneled cell for synthesis monitoring (MICCS) NMR analysis, revealed that anti‐aldol adducts were formed at the initial stage of the reactions under kinetic control, but the final products were the trans‐(syn)‐N,O‐acetal adducts that were produced through a retro‐aldol process under thermodynamic control. In the whole reaction process, the zinc catalyst played three important roles: i) promotion of the aldol process (C?C bond formation), ii) cyclization process to the N,O‐acetal product (C?O bond formation), and iii) retro‐aldol process from the anti‐aldol adduct to the syn‐aldol adduct (C?C bond cleavage and C?C bond formation).     

Novel reactions of arylmalonate carbanions. The reaction with phenyl isocyanate resulting in carbamates by 1,3-C→N migration of the ethoxycarbonyl group

The reactions of carbanions of diethyl phenyl and 4-nitrophenylmalonates with phenyl isocyanate occur with 1,3-C→N migration of the ethoxycarbonyl group to form the corresponding adducts. The introduction of NO₂ groups into the benzene ring of arylmalonates inhibits the reaction. Dedicated to Academician V. A. Tartakovsky on the occasion of his 75th birthday. Published in Russian in Izvestiya Akademii Nauk. Seriya Khimicheskaya, No. 8, pp. 1608–1610, August, 2007.