19F and 1H NMR of aldimines of fluoroamino acids with pyridoxal-5′-phosphate

¹H and ¹⁹F NMR spectra were obtained for six Schiff bases (aldimines) formed by pyridoxal-5′-phosphate (PLP) with four fluorinated or their two parent non-fluorinated α-amino acids (phenylalanine and α-aminobutyric acid). pK_A Values were derived from ¹H and ¹⁹F titration curves. The imine nitrogen of the aldimines is very basic (～13) and sensitive to the electron withdrawing effect of fluorine. The pyridine nitrogen is less basic in the aldimines (～7) than in PLP (8.12) and is less sensitive to the electron withdrawing effect of the fluorine than is the imine nitrogen. The phosphate group has a pK in the same range (～6) and the chemical shifts of some nuclei are sensitive to both pK values. Protonation of the aldimine causes the ¹H signal to shift downfield at the methyl protons of the pyridine ring and at the aldehydic proton of the aldimine for the high pK value (except for the aldimines prepared from the β-fluorophenylalanine), but upfield at the aromatic proton and at the aldehydic proton of the aldimine for the low pK. Protonation of the aldimine causes the ¹⁹F signal of an aryl fluorine to shift downfield but gives an upfield shift at a β-fluorine. These data are related to the highly conjugated electronic structure of the Schiff bases.     

Chemoselective Synthesis of β‐Amino Ester or β‐Lactam via Sonochemical Reformatsky Reaction

A series of β‐amino esters were synthesized by the reaction of N‐tosyl aldimine or N‐hydroxy aldimine with bromoacetate by sonochemical Reformatsky reaction. The β‐N‐hydroxyamino ester was obtained and the formed sensitive hydroxylamino functionality was resistant under the reaction condition. The β‐lactam also was synthesized by the reaction of N‐p‐methoxy aldimine as reacting substrate under this sonochemical Reformatsky reaction condition.     

Rh(I)-catalyzed addition of alkenylzirconocene chlorides to aldimine derivatives

[RhCl(COD)]₂ (2 mol%) catalyzed reactions of alkenylzirconocene chloride complexes to N-Ts, -PO(OEt)₂ and COOR aldimine derivatives were efficiently carried out in dioxane at room temperature to give allylic amine derivatives in excellent yields. This is the first example of the catalytic addition reactions of alkenylzirconocene chloride complexes to aldimine derivatives.     

Tridentate anilido‐aldimine magnesium and zinc complexes as efficient catalysts for ring‐opening polymerization of ε‐caprolactone and L‐lactide

A novel tridentate anilido‐aldimine ligand, [o‐C₆H₄(NHAr)? HC?NCH₂CH₂NMe₂] (Ar = 2,6‐ⁱPr₂C₆H₃, L ‐H, 1 ), has been prepared by the condensation of N, N‐dimethylethylenediamine with one molar equivalent of 2‐fluoro‐benzaldehyde in hexane, followed by the addition of the lithium salt of diisopropylaniline in THF. Magnesium (Mg) and zinc (Zn) complexes supported by the tridentate anilido‐aldimine ligand have been synthesized and structurally characterized. Reaction of L ‐H ( 1 ) with an equivalent amount of MgⁿBu₂ or ZnEt₂ produces the monomeric complex [ L MgⁿBu] ( 2 ) or [ L ZnEt] ( 3 ), respectively. Experimental results show that complexes 2 and 3 are efficient catalysts for ring‐opening polymerization of ε‐caprolactone (CL) and L ‐lactide (LA) in the presence of benzyl alcohol and catalyze the polymerization of ε‐CL and L ‐LA in a controlled fashion yielding polymers with a narrow polydispersity index. In both polymerizations, the activity of Mg complex 2 is higher than that of Zn complex 3 , which is probably due to the higher Lewis acidity and better oxophilic nature of Mg²⁺ metal. © 2009 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 47: 4927–4936, 2009     

Condensation of pyridoxal with the methyl ester of glycine

Condensation of pyridoxal with the methyl ester of glycine gave the aminocoumarin analog 3-amino-8-rnethyl-2-oxo-2H-pyrano[2,3-c]pyridine-5-methanol (III), and not the expected aldimine. The structure of the compound was deduced by independent synthesis and by comparing its NMR spectrum with that of 3-aminocoumarin. The new reaction provides routes for the synthesis of α⁴-pyridoxylideneglycine and α⁴-pyridoxyloxoacetic acid derivatives. It may also provide a model for irreversible inactivation of vitamin B₆ in biochemical systems.     

Rhenium-catalyzed insertion of terminal alkenes into a C(sp)-H bond and successive transfer hydrogenation

Treatment of aromatic aldimines with terminal alkenes in the presence of a rhenium catalyst, [HRe(CO)₄]_n, gives 2-alkenylbenzylamines in good to excellent yields. This reaction proceeds via the insertion of the alkene into a C-H bond at the ortho-position of the imino group of the aromatic aldimine followed by sequential β-hydride elimination from the formed alkyl rhenium intermediate and then by hydrogenation of the imino group of the aldimine.     

Dioxygen Activation by Redox-Active Bis(aldimine) Ligand Bridged Diruthenium Complex Possessing Singlet Ground State

The unexplored ‘actor’ behavior of redox-active bis(aldimine) congener, p-phenylene-bis(picoline)aldimine (L1), towards dioxygen activation and subsequent functionalization of its backbone was demonstrated on coordination with {Ru(acac)₂} (acac= acetylacetonate). Reaction under aerobic condition led to the one-pot generation of dinuclear complexes with unperturbed L1, imino-carboxamido (L2⁻), and bis(carboxamido) (L3²⁻)-bridged isovalent {Ru^II(μ-L1)Ru^II}, 1/ {Ru^III(μ-L3²⁻)Ru^III}, 3 and mixed-valent {Ru^II(μ-L2⁻)Ru^III}, 2 . Authentication of the complexes along with the redox non-innocence behavior of their bridge have been validated through structure, spectroelectrochemistry and DFT calculations. Kinetic and isotope labelling experiments together with DFT analyzed transition states justified the consideration of redox shuttling at metal/L1 interface for ³O₂ activation despite of the closed shell configuration of 1 (S=0) to give carboxamido derived 2 / 3 .     

Theoretical and X-ray Crystallographic Evidence of a Fluorine-Imine Gauche Effect: An Addendum to Dunathan's Stereoelectronic Hypothesis

The preference of β‐fluoroimines to adopt a gauche conformation has been studied by single‐crystal X‐ray diffraction analysis and DFT methods. Empirical and theoretical evidence for a preferential gauche arrangement around the NCCF torsion angle (?) is presented ((E)‐2‐fluoro‐N‐(4‐nitrobenzylidene)ethanamine: ?_NCCF=70.0°). In the context of this study, the analysis of a pyridoxal‐derived β‐fluoroaldimine was performed, a species that is implicated in the inhibition of pyridoxal phosphate (PLP)‐dependent enzymes by β‐fluoroamine derivatives. The gauche preference of the internal aldimine (=NCH₂CH₂F) that can be rationalized by stereoelectronic arguments does not hold for the corresponding external system (N?CHCH₂F) (E_min when ?_NCCF=120°). Moreover, the C? F bond is lengthened by more than 0.02 Å at ?_NCCF=±90°, when it is exactly antiperiplanar to the conjugated imine. This activation of the C? F σ bond by an adjacent π system constitutes an addendum to Dunathan’s stereoelectronic hypothesis.     

Synthesis and Reactions of the Novel Diphosphine,iPrN = C[CH2P(NiPr2)2]2

Abstract

The aldimine nBuN=CHiPr and phosphorus trichloride react to give phosphorus(III) amides in a 1:1 and 2:1 molar ratio. An imine-enamine tautomerism is proposed. In a [4+1] cycloaddition reaction diacetyl-(N-n-butyl)diimine and λ³σ³P-species, RPCl₂ or EtOPCl₂, form 1,2,3λ⁵σ⁴ -diazaphospholenes¹. The same diimine and (Et₂N)₂ PCl is furnishing annellated azaphospholenes¹. A 1,3,4λ⁵ σ⁴ -diazaphospholanium is formed from a λ³σ³ -phosphenium and iPrN=CMe₂ ². Phosphorus(III) amides P(NR₂)₃ (R= Me, Et) and O-trimethylsilylated diacetyldioxime give rise to yield the first monocyclic pentaazaphosphoranes.     

Synthesis of novel P-ketimine bidentate ferrocenyl ligands with central and planar chirality and comparsion in the catalytic activity between P-ketimine and P-aldimine

A series of novel ferrocenylphosphine-ketimine ligands 6 were prepared by reaction of (R,S_p)-PPFNH₂-R or (S,S_p)-PPFNH₂ with a variety of m-substituted acetophenones. A different catalytic activity was observed between ferrocenylphosphine-ketimine ligands and corresponding aldimine ligands. The efficiency and diastereomeric impact of these ferrocenylphosphine-ketimine ligands in Pd-catalyzed asymmetric allylic alkylation were first investigated, and higher enantioselectivity of over 98% e.e. with 95% yield was obtained by the use of ferrocenylphosphine-ketimine ligands. However, in Rh-catalyzed asymmetric hydrosilylation of aryl ketones, only 42% e.e. was obtained by the use of ferrocenylphosphine-ketimine ligands compared to 90% e.e. with the use of aldimine ligands.     

Synthesis of N-(Dimethylsulfamoyl)aldimines,a New Type of Aldimine Derivative

N-(Dimethylsulfamoyl)aldimines (3) a new type of shelf-stable aldimine derivatives, are readily prepared from aldehydes and N-(dimethylsulfamoyl)amide (2) in refluxing toluene.     

Fluoroimines from the reaction of fluoro amino acids or fluoroketo acids with the aldehyde or amine form of vitamin B6: 2—Stereochemical aspects of their formation from β-fluoroaspartates or β-fluorooxaloacetate,using 19F NMR

The fluorine NMR spectra of systems initially containing 0.05–0.1 M of pyridoxal 5′-phosphate and erythro-β-fluoroaspartate (or threo-β-fluoroaspartate) in D₂O solution were examined over the pD range 1–12. The formation of the aldimine Schiff base gave only one stereoisomer, whcih was trapped with sodium borohydride. Reactions of pyriodoxamine 5′-phosphate and fluorooxaloacetate were examined under the same conditions. A mixture of two products was given, identified as two ketimine Schiff bases (E and Z isomers) with well characterized fluorine chemical shifts and ²J(DF) values. This mixture, trapped with sodium borohydride, gives the two reduced erythro and threo aldimines. The configurations and conformations of all reaction products were determined using the ³J(HF) values and their correlation with the fluorine chemical shift. The role of the 3-phenolate oxygen of the pyridine ring, of the conjugate acid of the iminium nitrogen and of the carboxylate oxygen in ionic or hydrogen bond interactions in the determination of the stereochemistry is discussed.     

Synthesis of syn-vicinal diamines via the stereoselective allylation of acyclic chiral α-amino aldimines

The stereoselective allylation of acyclic chiral α-amino aldimines affording vicinal diamines, mediated by various Lewis acids (TiCl₄, SnCl₄, MgBr₂·OEt₂, BF₃·OEt₂, ZnCl₂), is described. The TiCl₄-mediated allylation of an α-N-Boc aldimine afforded the allylation product with syn-selectivity, which in turn was used for the synthesis of an intermediate of an oseltamivir derivative.     

Neue ONS‐Liganden und ihre Zinkkomplexe mit Bezug zum Zinkenzym Alkoholdehydrogenase

New ONS Ligands and their Zinc Complexes with Relation to the Zinc Enzyme Alcoholdehydrogenase By ring opening of dimethyl thiirane with ethanolamine or by Schiff base condensation between salicylic aldehydes and 2‐mercaptoisobutylamine the tridentate ONS ligands H₂MIEA, H₂MIIMP, and H₂MIIMTP were obtained. The former yielded the zinc complex (MIEA)Zn(ethanolamine) ( 1 ) with a trigonal bipyramidal ZnO₂N₂S coordination. The latter two and Zn[N(SiMe₃)₂]₂ yielded the presumably dimeric complexes Zn(MIIMP) and Zn(MIIMTP) ( 2 a , b ). Benzoyl pyridine and phenylhydroxymethylpyridine as bidentate coligands L could be combined with H₂MIIMP in the complexes L · Zn(MIIMP) ( 3 , 4 ) whose ZnO₂N₂S coordination corresponds to that of 1 . Partial hydrolytic degradation led to the unusual trinuclear complex 5 which contains, inter alia, the condensation product of the salicylic aldimine and benzoyl pyridine as a ligand. The complexes obtained and the coordination patterns observed represent new structural analogies with the environment of zinc in the enzyme horse liver alcoholdehydrogenase.     

Ring‐opening polymerization of β‐butyrolactone catalyzed by efficient magnesium and zinc complexes derived from tridentate anilido‐aldimine ligand

Magnesium (Mg) and zinc (Zn) complexes incorporating tridentate anilido‐aldimine ligand, (E)‐2, 6‐diisopropyl‐N‐(2‐((2‐(piperidin‐1‐yl)ethylimino)methyl)phenyl)aniline ( AA ^Pip ‐H, 1 ), were synthesized and structurally characterized. The reaction of AA ^Pip ‐H ( 1 ) with MgⁿBu₂ or ZnEt₂ in equivalent proportions afforded the monomeric complex [( AA ^Pip )MgⁿBu] ( 2 ) or [( AA ^Pip )ZnEt] ( 3 ), respectively. The coordination modes of these complexes differ in the solid state: Mg complex 2 shows a four‐coordinated and distorted tetrahedral geometry, whereas Zn complex 3 adopts a trigonal planar geometry with a three‐coordinated Zn center. Complexes 2 and 3 are efficient catalysts for the ring‐opening polymerization of β‐butyrolactone (β‐BL) in the presence of 9‐anthracenemethanol (9‐AnOH). The polymerization of β‐BL with the Zn catalyst system is demonstrated in a living fashion with a narrow polydispersity index, PDI = 1.01–1.10. The number‐averaged molecular weight (M_n) of the produced poly(3‐hydroxybutyrate) (PHB) is quite close to the expected M_n over diverse molar ratios of monomer to 9‐AnOH. A greater ratio of monomer to alcohol catalyzed by Zn complex 3 served to form PHB with a large molecular weight (M_n > 60000). An effective method to prepare PHB‐b‐PCL and PEG‐b‐PHB by the ring‐opening copolymerization of β‐BL catalyzed by zinc complex 3 is reported. © 2010 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem, 2010     

Synthesis of cis-3,4-diaryl α-methylene-γ-butyrolactams via sonochemical Barbier-type reaction

A series of cis-3,4-diaryl α-methylene-γ-butyrolactams were synthesized by the addition reaction of 3-phenylallyl bromide with N-tosyl aldimine via sonochemical Barbier-type reaction condition and then followed by the in situ intramolecular amidation. The cis-3,4-diaryl α-methylene-γ-butyrolactam was obtained as the sole regio- and stereoisomeric product when N-tosyl aldimine was used as the substrate whereas the monoaryl α-methylene-γ-butyrolactam was also generated when N-phenyl aldimine was used.     

Lewis Acid or Brønsted Acid Catalyzed Reactions of Vinylidene Cyclopropanes with Activated Carbon–Nitrogen,Nitrogen–Nitrogen,and Iodine–Nitrogen Double‐Bond‐Containing Compounds

Lewis acid or Brønsted acid catalyzed reactions of vinylidene cyclopropanes (VDCPs), 1 , with activated carbon–nitrogen, nitrogen–nitrogen, and iodine–nitrogen double‐bond‐containing compounds have been thoroughly investigated. We found that pyrrolidine and 1,2,3,4‐tetrahydroquinoline derivatives can be formed in good yields in the reactions of VDCPs 1 with ethyl (arylimino)acetates 2 by a [3+2] cycloaddition or intramolecular Friedel–Crafts reaction pathway. Based on these results, we found that activated carbon–nitrogen and nitrogen–nitrogen double‐bond‐containing compounds, such as N‐toluene‐4‐sulfonyl (N‐Ts) imines 5 and diisopropylazodicarboxylate ( 7 ), can also react with VDCPs 1 to give [3+2] cycloaddition products in moderate to good yields in the presence of a Lewis acid. When N‐tert‐butoxycarbonyl aldimine 9 was used as the substrate, six‐membered cycloaddition products 10 and 11 were formed in moderate yields in the presence of a Brønsted acid, trifluoromethanesulfonic acid (TfOH). The reactions of VDCPs 1 with N‐Ts‐iminophenyliodinane ( 12 ) were also carried out in the presence of (CuOTf)₂ ? C₆H₆ and it was found that nitrogen‐containing indene derivatives 13 were obtained, rather than the aziridination products. Plausible mechanisms for all of these transformations are discussed, based on the obtained results.     

Stereoselective allylation of α-hydroxy aldimines and its application to the formal synthesis of (−)-β-conhydrine

Stereoselective allylation of N-p-methoxyphenyl (PMP)-substituted α-hydroxy aldimines is described. Several Lewis acids (BF₃·OEt₂, SnCl₄, TiCl₄, ZnCl₂, and MgBr₂·OEt₂) were employed to mediate the allylation reactions. The addition of the allyl group generates a new stereocenter and affords the syn vicinal amino alcohol. Formal synthesis of (?)-β-conhydrine (1) was accomplished via syn-selective allyl addition to N-PMP-substituted α-hydroxy aldimine.     

Potential inhibitors of DNA topoisomerase II: ruthenium(II) poly-pyridyl and pyridyl-azine complexes

In search of new DNA probes a series of new mono and binuclear cationic complexes [RuH(CO)(PPh₃)₂(L)]⁺ and [RuH(CO)(PPh₃)₂(-μ-L)RuH(CO)(PPh₃)₂]²⁺ [L=pyridine-2-carbaldehyde azine (paa), p-phenylene-bis(picoline)aldimine (pbp) and p-biphenylene-bis(picoline)aldimine (bbp)] have been synthesized. The reaction products were characterized by microanalyses, spectral (IR, UV-Vis, NMR and ESMS and FAB-MS) and electrochemical studies. Structure of the representative mononuclear complex [RuH(CO)(PPh₃)₂(paa)]BF₄ was crystallographically determined. The crystal packing in the complex [RuH(CO)(PPh₃)₂(paa)]BF₄ is stabilized by intermolecular π-π stacking resulting into a spiral network. Topoisomerase II inhibitory activity of the complexes and a few other related complexes [RuH(CO)(PPh₃)₂(L)]⁺ {L=2,4,6-tris(2-pyridyl)-1,3,5-triazine (tptz) and 2,3-bis(2-pyridyl)-pyrazine (bppz)} have been examined against filarial parasite Setaria cervi. Absorption titration experiments provided good support for DNA interaction and binding constants have also been calculated which were found in the range 1.2 × 10³-4.01 × 10⁴ M⁻¹.     

Vibrational spectra of N-2′-methyl-propyliden-propan-2-amine: conformational analysis and influence of the nitrogen hybridization

Infrared and Raman spectra of the (CH₃)₂C^2′HC^1′HNCH(CH₃)₂ aldimine (NPP) and of two deuterated derivatives at C^1′ and C^2′ in the liquid, solid and solution phases have been recorded and assigned between 4000 and 130 cm⁻¹. NPP adopts the E configuration and two conformers at the C_sp2 and N sides are in equilibrium. Some vibrational modes are specifically assigned to the anticlinal (ac) or synperiplanar (sp) conformers at the C_sp2 side. The ac(C_sp2) form is dominant in the pure liquid whilst the sp(C_sp2) form is favoured in the solid and in chloroform. The vibrational dynamics of the isopropyl group on both sides of the CN bond are partially similar to that of the (CH₃)₂CHCHO aldehyde on the one hand and of the (CH₃)₂CHNH₂ amine on the other hand. When moving from the amine to the corresponding aldimine, changes about νNC and wCC₂ modes (at the N side) are related to electronic and geometrical effects as a consequence of the nitrogen hybridization change from sp₃ to sp₂.