Preparation of N-alkylbis(3-aminopropyl)amines by the catalytic hydrogenation of N-alkylbis(cyanoethyl)amines

An improved process for the preparation of N-alkylbis(3-aminopropyl)amines is described. These triamines are of interest as monomers for the condensation polymerization with esterified carbohydrate diacids (aldaric acids) to generate the corresponding poly(4-alkyl-4-azaheptamethylene aldaramides). The triamine synthesis is comprised of two efficient steps and requires no chromatographic purification. Bisconjugate addition of alkylamines to acrylonitrile followed by catalytic hydrogenation of the N-alkylbis(cyanoethyl)amines over Raney nickel yields the target N-alkylbis(3-aminopropyl)amines. Much less solvent was used in the bisconjugate addition step then previously reported, and in the second step, a relatively low-pressure catalytic hydrogenation (50 psi of hydrogen) was employed using Raney nickel as the catalyst in a 7 N methanolic ammonia solvent system to afford the N-alkylbis(3-aminopropyl)amines of high purity in nearly quantitative yield.     

A convergent synthesis of Hexahomotriazacalix

A new, convergent synthesis of hexahomotriazacalix[3]arenes 1a-e is described. The key transformation in this synthesis involves the coupling of the triamines 4a-d with 2, 6-bis(chloromethyl)-4-methylphenol 5 and results in the formation of the hexahomotriazacalix[3]arenes 1a-d in 90-95% yield. The triamines 4a-d were constructed by the one-pot reaction of monochloroaldehyde 3 and a primary amine followed by reduction to yield the triamines 4a-d in 50-55% yield. Deallylation of macrocycle 1d was accomplished by palladium catalysis to obtain the N-unsubstituted macrocycle 1e, which has the potential to be a precursor to a variety of N-substituted hexahomotriazacalix[3]arenes.     

Screening of a combinatorial library of synthetic polyamines displaying selectivity in multiple ion-pairing interactions with model polyanionic compounds in aqueous organic solutions

The biological activity of natural polyamines is due in large part to their ability to form ion-pairing interactions with polyanionic biomolecules, such as proteins, oligonucleotides, and sulfated oligosaccharides. Unfortunately, the diversity of biogenic polyamines is compromised by their limitation to only just a few internitrogen spacers. As a proof-of-principle study, a synthetic split-pool library of linear triamines was screened in an on-bead assay against a selection of model trisulfonated azo dyes (1, 2, and 3) and a short glutamate-rich nonameric peptide (4) to demonstrate its use in the discovery of selective ligands via multivalent ion pairing. From screening a 196-membered split-pool library against the dyes in aqueous organic solutions, with or without spermidine as competing ligand, it was found that the most frequent residues possessed internitrogen distances that were very similar to the sulfonate distances on the dyes. The results from these screening assays were used in the design of two polyamine sequences (8, 8Aoc(R)-8Aoc(R), and 12, 2Acc(R)-epsilonAhx(R)) for follow-up studies in solution phase. These triamines demonstrated the same selectively toward dyes 2 and 3 as observed by the solid-phase approach. In addition, resin-supported triamines, synthesized as discrete compounds, were able to selectively extract either dye 2 or 3 from a mixture of the two, further verifying the observations made from the library screening efforts. With peptide 4, containing three glutamate residues, a preference was found for rather long residues (12 and 8 carbons long), which is suggestive of a linear peptide, rather than a helical motif under the conditions of the screening.     

Convenient preparation of optically active N,N-bis(4-substituted-4-aminobutyl)amines

An efficient and convenient method for the synthesis of chiral triamines with two substituents at the α position to the terminal amino group (spermidine analogues) is described. These chiral N,N-bis(4-substituted-4-aminobutyl)amines may have anticancer activities.     

1,4-dicyanobenzene as a scaffold for the preparation of bimetallic actinide complexes exhibiting metal-metal communication

Reaction of two equivalents of [(C(5)Me(4)Et)(2)U(CH(3))(Cl)] (6) or [(C(5)Me(5))(2)Th(CH(3))(Br)] (7) with 1,4-dicyanobenzene leads to the formation of the novel 1,4-phenylenediketimide-bridged bimetallic organoactinide complexes [{(C(5)Me(4)Et)(2)(Cl)U}(2)(mu-{N==C(CH(3))-C(6)H(4)-(CH(3))C==N})] (8) and [{(C(5)Me(5))(2)(Br)Th}(2)(mu-{N==C(CH(3))-C(6)H(4)- (CH(3))C==N})] (9), respectively. These complexes were structurally characterized by single-crystal X-ray diffraction and NMR spectroscopy. Metal-metal interactions in these isovalent bimetallic systems were assessed by means of cyclic voltammetry, UV-visible/NIR absorption spectroscopy, and variable-temperature magnetic susceptibility. Although evidence for magnetic coupling between metal centers in the bimetallic U(IV)/U(IV) (5f(2)-5f(2)) complex is ambiguous, the complex displays appreciable electronic communication between the metal centers through the pi system of the dianionic diketimide bridging ligand, as judged by voltammetry. The transition intensities of the f-f bands for the bimetallic U(IV)/U(IV) system decrease substantially compared to the related monometallic ketimide chloride complex, [(C(5)Me(5))(2)U(Cl){-N==C(CH(3))-(3,4,5-F(3)-C(6)H(2))}] (11). Also reported herein are new synthetic routes to the actinide starting materials [(C(5)Me(4)Et)(2)U(CH(3))(Cl)] (6) and [(C(5)Me(5))(2)Th(CH(3))(Br)] (7) in addition to the syntheses and structures of the monometallic uranium complexes [(C(5)Me(4)Et)(2)UCl(2)] (3), [(C(5)Me(4)Et)(2)U(CH(3))(2)] (4), [(C(5)Me(4)Et)(2)U{-N==C(CH(3))-C(6)H(4)-C==N}(2)] (10), and 11.     

Polysiloxane-Immobilized Triamine Ligand System,Synthesis and Applications

The polysiloxane-immobilized triamine ligand system of the formula P-(CH 2 ) 3 NH(CH 2 ) 2 NH(CH 2 ) 2 NH 2 (where P represents the siloxane network) has been prepared via the sol-gel process by hydrolytic polycondensation of (EtO) 4 Si and (MeO) 3 Si(CH 2 ) 3 NH(CH 2 ) 2 NH(CH 2 ) 2 NH 2 . An alternative method was used by the reaction of the iodopolysiloxane P-(CH 2 ) 3 -I and diethylenetriamine in the presence of triethylamine. The immobilized triamine ligand forms metal chelate complexes when treated with aqueous metal(II) ion solutions (Co 2+ , Ni 2+ , and Cu 2+ ). The elemental analysis and FTIR results suggest that this ligand system undergoes a substantial leaching of diethylenetriamine ligand moieties from the siloxane framework.     

Na+ and Mg2+ ion effect on the stability of a poly I . poly A . poly I triple helix

Differential UV spectroscopy was used to study the temperature dependence of the conformational equilibrium in aqueous poly I . poly A . poly I (A2I) solutions containing Na+ (0.1-2 M) and Mg2+ (10(-5)-0.005 M) ions. Over the whole range of the studied Na+ and Mg2+ concentrations, the heating-induced destruction of the triple A2I helix is actually the A2I --> A + I + I (3 --> 1) transition. The rise of the transition temperature with increasing Na+ and Mg2+ contents is well described by Manning's and the "ligand" theories, which makes it possible to estimate the linear charge density on the single-stranded poly I (xi = 1.9 +/- 0.1) and the Mg2+-A2I binding constant (K = 1,250 M(-1) for the zero degree of binding). An analytical expression has been obtained, which correlates the constants of Mg2+ binding to three- and single-stranded polynucleotides (K3 and K1, respectively) and the linear charge density on them. There are only minor distinctions between the K3 values for A2U and A2I because these polynucleotides have similar structures. The difference in the K1 values is also slight as single-stranded poly U, poly I, and poly A have similar conformations. Dependence of the conformational transition temperatures of two triple helices with changing Mg2+ concentration.     

Dinuclear platinum complexes with biological relevance based on the 1,2-diaminocyclohexane carrier ligand

The synthesis of bifunctional dinuclear platinum complexes, [{PtCl(dach)}(2)-mu-Y](n+)Cl(n) (1-3; Y = H(2)N(CH(2))(3)NH(2)(CH(2))(4)NH(2), H(2)N(CH(2))(6)NH(2)(CH(2))(6)NH(2), and H(2)N(CH(2))(6)NH(2)(CH(2))(2)NH(2)(CH(2))(6)NH(2), respectively; Figure 1) is reported. There was no labilization of the polyamine linker groups of the cis-1,2-diaminocyclohexane complexes in the presence of sulfur-containing species at physiological pH, in contrast to previous studies preformed on trans complexes. Metabolism reactions are somewhat dependent on the nature of the polyamine: at physiological pH, the spermidine complex 1 forms an inert (tetraamine)platinum species in which one platinum is chelated by a central and terminal amino group. The stability of cis-geometry complexes may make them viable second-generation polynuclear platinum clinical candidates.     

Capillary gas-chromatographic determination of spermidine in hair lotion

Biogenic polyamines, such as spermidine (SPD, NH2-(CH2)4-NH-(CH2)3-NH2), are ubiquitous polycationic molecules which play a definitive role in many biological processes such as nucleic acid metabolism, protein synthesis, and cell growth. SPD is commonly used as an ingredient in hair lotions, because it seems to promote hair growth. This work describes a capillary GC method for quantitative determination of SPD in hair lotions using 1,6-diaminohexane as internal standard, a methyl silicone capillary column, and a flame ionisation detector. Aliquots of hair lotion were treated with an alkaline aqueous solution and internal standard was added. The emulsion was extracted with diethyl ether containing ethyl chloroformate. Ether extracts, evaporated to dryness and reconstituted in ethyl acetate, were analysed by capillary GC with flame ionisation detection. Validation took into account the specificity, linearity, precision, and accuracy of the analytical method: these parameters were valid for the quantitative determination of SPD in hair lotion.     

Electrospray ionization mass spectra of monoimidazole/polyamine conjugates

Imidazole/polyamine amides are biologically important molecules due to their specific DNA binding activity, and much attention has been attracted to the synthesis of their derivatives or analogues. In the present studies, the fragmentation of a series of synthetic monoimidazole/polyamine amides was investigated using electrospray ionization mass spectrometry (ESI-MS) combined with tandem mass spectrometry (ESI-MS/MS). All of the monoimidazole/polyamine amides produced the fragment ion m/z 183 except for the monoimidazole/ethyldiamine amide. The diamine amides produced this ion after the elimination of an alkene, the triamine amides produced it via their corresponding diamine amide fragments, and the tetraamine amide via its triamine and then diamine amide fragments. The characterization of the mass spectra for the different polyamine amides allowed identification of a specific product from the N-acylation of spermidine, and should assist further study of the polyamine amides in DNA binding action.     

Synthesis and structure of diamido ether uranium(IV) and thorium(IV) halide "ate" complexes and their conversion to salt-free bis(alkyl) complexes

The high-yield synthesis, spectroscopic and structural determination of three new uranium(IV) and thorium(IV)ate complexes supported by three different diamido ether ligands are reported. The reaction of Li2[2,6-iPr2PhN(CH2CH2)]2O (Li2[DIPPNCOCN]) with 1 equiv. of UCl4 in THF generates [DIPPNCOCN]UCl3Li(THF)2(1), while reaction in toluene/ether gives salt-free [DIPPNCOCN]UCl2.1/2C7H8(2), which was identified by paramagnetically shifted 1H NMR. Reaction of 0.5 equiv. of {[tBuNON]UCl2}2([tBuNON]=[(CH3)3CN(Si(CH3)2)]2O2-) with 3.5 equiv. LiI in toluene and a minimal amount of THF results in [tBuNON]UI3Li(THF)2(3) and is very similar in structure to 1. {[MesNON]ThCl3Li(THF)}2(4), a dimeric complex with a Th2Li2Cl6 core, is prepared by reaction of Li2[2,4,6-Me3PhN(Si(CH3)2)]2O (Li2[MesNON]) with ThCl4 in THF. The analogous reaction in toluene did not yield the salt-free complex but rather a sterically crowded diligated compound, [MesNON]2Th (5), which was also structurally characterized. Complex 5 was prepared rationally by reacting 2 equiv. Li2[MesNON] with ThCl4 in toluene. The reaction of 1 and 3 with 2 equiv. of LiCH2Si(CH3)3 generates the stable, salt-free organoactinides [DIPPNCOCN]U(CH2Si(CH3)3)2(6) and [tBuNON]U(CH2Si(CH3)3)2(7). Complex 6 was structurally characterized. These reactions illustrate the viability of ate complexes as useful synthetic precursors.     

DNA and RNA noncovalent interaction of platinum(II) polypyridine complexes

A comparative investigation of the noncovalent interaction of the platinum(II) polypyridine complexes [Pt(dipy)(n-Rpy)2]2+ and [Pt(4,4'-Me2dipy)(2-Rpy)2]2+ (dipy = 2,2'-dipyridine; Me = CH3; n = 2-4; R = H or CH3) with double-helical DNA (calf thymus) and RNA [poly(A).poly(U)] has been conducted. With the exception of [Pt(dipy)(2-Mepy)2]2+, all of the complexes interact strongly, by intercalation, with both nucleic acids giving rise to large changes in the electronic spectra and induced circular dichroism signals; in addition, viscosity experiments on rodlike DNA and RNA show that both biopolymers elongate upon interaction with the complexes. The binding constant values, KB, determined at 25 degrees C, indicate that, at 0.101 M ionic strength, the affinity for poly(A).poly(U) is strongly dependent on the complexes nature, while for DNA it is leveled off. [Pt(dipy)(2-Mepy)2]2+ binds to DNA but does not interact appreciably with poly(A).poly(U).     

Alkaline ribonuclease associated with polyribosomes in fibroblasts of experimental granulation tissue.

Alkaline ribonuclease (RNase) from polyribosomes derived from experimental granulation tissue has been purified 1900-fold through affinity chromatography. The preparation was homogeneous in sodium dodecyl sulfate (SDS) polyacrylamide-gel electrophoresis with an estimated molecular weight of 15 000. Purified RNase was completely inhibited in the presence of divalent ions Mg2+(100 mM) and Ca2+(100 mM) but activated slightly with Na+(50 mM). The enzyme is an endonuclease and the best substrates were poly(U), mixed RNA from yeast, rRNA from granulation tissue and poly(C). The estimated apparent Km-values were 0.037, 0.064, 0.13 and 0.27 g1-1, respectively. In polyribosomes RNase occurred in both free and p-chloromercuribenzoate (pCMB)-liberated forms. The total activity was at the highest but the proportion of the free activity minimal in the granulation tissue during the maximal synthesis of collagen.     

Highly efficient "grafting from" an α-helical polypeptide backbone by atom transfer radical polymerization

Because of their favorable biodegradability, biocompatibility, regular secondary structures, and stimuli‐responsiveness, synthetic polypeptides have attracted more and more attention in the biomedical material field. In this work, a novel thermo‐responsive graft polypeptide, poly(L ‐glutamate)‐graft‐poly(2‐(2‐methoxyethoxy)ethyl methacrylate) (PLG‐g‐PMEO₂MA), is prepared through a combination of ring‐opening polymerization and atom transfer radical polymerization. The structure of PLG‐g‐PMEO₂MA is confirmed by FT‐IR, ¹H NMR, and GPC analyses. The phase transition temperature of PLG‐g‐PMEO₂MA is adjustable by varying the NaCl concentration in aqueous solution. PLG‐g‐PMEO₂MA adopts α‐helical conformations both in aqueous solution at 25 and 60 °C and even in the solid state. In addition, PLG‐g‐PMEO₂MA forms stimuli‐responsive micelles with an α‐helical core and a thermo‐responsive shell in water.

     

Intramolecular and intermolecular N-H...C(5)H(5)(-) hydrogen bonding in magnesocene adducts of alkylamines. Implications for chemical vapor deposition using cyclopentadienyl source compounds

Magnesocene adducts of alkylamines were prepared and characterized. Treatment of 3-amino-2,4-dimethylpentane, isopropylamine, tert-butylamine, benzylamine, or N-isopropylbenzylamine with magnesocene at ambient temperature in toluene afforded the amine adducts Cp2Mg(NH2CH(CH(CH3)2)2) (91%), Cp2Mg(NH2iPr) (80%), Cp2Mg(NH2tBu) (67%), Cp2Mg(NH2CH2Ph) (80%), and Cp2Mg(NH(CH(CH3)2)(CH2C6H5)) (91%). These adducts are stable at ambient temperature, and Cp2Mg(NH2CH(CH(CH3)2)2) can be sublimed at 60 degrees C/0.05 Torr without any evidence for reversion to magnesocene. The solid-state structure of Cp2Mg(NH2CH(CH(CH3)2)2) contains eta5- and eta2-cyclopentadienyl ligands, and the hydrogen atoms on the coordinated amine nitrogen atom participate in intramolecular and intermolecular hydrogen bonding to the eta2-cyclopentadienyl ligand. The observed hydrogen bonding is relevant to the path by which cyclopentadiene is eliminated from metal cyclopentadienyl CVD source compounds during film growth employing acidic element hydrides as co-reactants.     

Design of an organocatalyst for the enantioselective Diels-Alder reaction with alpha-acyloxyacroleins

We have realized the first enantioselective organocatalytic Diels-Alder reaction between alpha-substituted acroleins, such as alpha-acyloxyacroleins, and not only cyclic but also acyclic dienes. alpha-Acyloxyacroleins are useful as synthetic equivalents of alpha-haloacroleins. The present catalyst could be prepared in situ from pentafluorobenzenesulfonic acid (2.5-3.0 equiv) and chiral triamine (1 equiv) derived from H-l-Phe-l-Leu-N(CH2CH2)2. The enantioselective Diels-Alder reaction of 5-(benzyloxymethyl)cyclopentadiene, cyclopentadiene, cyclohexadiene, 2,3-dimethylbutadiene, and isoprene with alpha-(p-methoxybenzoyloxy)acrolein catalyzed by the above chiral ammonium salt (2.5-20 mol %) at -20-22 degrees C gave the corresponding adducts with 83, 83, 91, 92, and 88% ee, respectively.     

The synthesis, structural, and spectroscopic characterization of uranium(IV) perrhenate complexes

We report the synthesis, structural, and spectroscopic characterization of a series of uranium(IV)-perrhenato complexes. Three isostructural complexes with general formula [U(ReO4)4(L)4] (where L = tri-n-butylphosphine oxide/TBPO (2), triethyl phosphate/TEP (3), or tri-iso-butyl phosphate/TiBP (4)), have been synthesized, both through the photoreduction of ethanolic {UO2}2+ solutions and also via a novel U(IV) starting material, U(ReO4)4.5H2O (1). Compound 1 has also been used in the preparation of [U(ReO4)4(TPPO)3(CH3CN)].2CH3CN (5) and [U(ReO4)(DPPMO2)3(OH)][ReO4]2.2CH3CN (6), where TPPO represents triphenylphosphine oxide and DPPMO2 represents bis(diphenylphosphino)methane dioxide. All six complexes have been spectroscopically characterized using NMR, UV-vis-NIR, and IR techniques, with 2, 3, 5, and 6 also fully structurally characterized. The U atoms in compounds 2-6 all exhibit eight-coordinate geometry with up to four perrhenate groups in addition to three (DPPMO2 and TPPO) or four (TEP, TiBP, TBPO) coordinated organic ligands. In the case of compounds 5 and 6, the coordination of eight ligands to the U(IV) center is completed by the binding of a solvent molecule (CH3CN) and OH-, respectively. Solid-state physical analysis (elemental and thermogravimetric) and infrared spectroscopy are in agreement with the structural studies. The crystallographic data suggest that the strength of the U(IV)-O-donor ligand bonds decreases across the series R3PO > [ReO4]- > (RO)3PO. Solution-state IR and 31P NMR spectroscopy appear to be in agreement with these solid-state results.     

Facile oxidation-based synthesis of sterically encumbered four-coordinate bis(2,9-di-tert-butyl-1,10-phenanthroline)copper(I) and related three-coordinate copper(I) complexes

A new oxidation-based synthetic route was developed for synthesis of Cu(I) complexes with weakly coordinating ligands, leading to the synthesis of the elusive [Cu(dtbp)2]+ (dtbp, 2,9-di-tert-butyl-1,10-phenanthroline) complex that may be useful as a sensor or as a dye for dye-sensitized solar cells. An acetone solution of either 1 or 2 equiv of dtbp was added to excess Cu(0) and 1 equiv of AgY (Y is O3SCF3-, BF4-, SbF6-, or B(C6F5)4-) in a nitrogen-filled glove box. Following filtration and evaporation under vacuum, crystallization from CH2Cl2 and hexanes results in X-ray quality crystals of Cu(dtbp)(O3SCF3) (1), Cu(dtbp)(BF4) (2), [Cu(dtbp)(acetone)][SbF6] (3), [Cu(dtbp)2][B(C6F5)4].CH2Cl2 (4.CH2Cl2), [Cu(dtbp)2][BF4].CH2Cl2 (5.CH2Cl2), and [Cu(dtbp)2][SbF6].CH2Cl2 (6.CH2Cl2). Complexes 1-6 were characterized by X-ray crystallography and NMR. The Cu atom in complexes 1-3 exhibited distorted trigonal coordination geometries, reflecting the steric effect of the bulky tert-butyl substituents. The structures of the pseudotetrahedral complexes 4, 4.CH2Cl2, 5.CH2Cl2, and 6.CH2Cl2 revealed the longest average Cu-N distances (2.11 A, 2.11 A, 2.10 A, and 2.11 A, respectively) in this class of compounds-longer by more than three standard deviations from the average.     

Synthetic and structural experiments on yttrium, cerium and magnesium trimethylsilylmethyls and their reaction products with nitriles; with a note on two cerium beta-diketiminates

The yttrium, cerium and magnesium bis(trimethylsilyl)methyls [Ln[CH(SiMe3)2]3][Ln = Y (1), Ce (2)], and the known compound Mg[[CH(SiMe3)2]2 (C) and [Mg(mu-Br)[CH(SiMe3)2](OEt2)]2 (D) formed the crystalline nitrile adducts [1(NCBut)2] (5), [2(NCPh)] (6), [C(NCR)2][R = But (8), Ph (9), C6H3Me2-2,6 (10)] and [Mg(mu-Br)[CH(SiMe3)2](NCR)]2 [R = But (11), Ph (12), C6H3Me2-2,6 (13)], rather than beta-diketiminato-metal insertion products. The beta-diketiminato-cerium complex [Ce[(N(SiMe3)C(C6H4But-4))2CH][N(SiMe3)2]2] (16) was obtained from [Ce[N(SiMe3)2]3] and the beta-diketimine H[[N(SiMe3)C(C6H4But-4)]2CH]]. The cerium alkyl 2 and [Ln[CH(SiMe3)(SiMe2OMe)]3][Ln = Y (3), Ce (4)] were obtained from the appropriate lithium alkyl precursor and [Ce(OC6H2But2-2,6-Me-4)3] or LnCl3, respectively. Heating complex 3 with benzonitrile in toluene afforded 2,2-dimethyl-4,6-diphenyl-5-trimethylsilyl-1,3-diaza-2-silahexa-1,3-diene (7), a member of a new class of heterocycles. The X-ray structures of the crystalline compounds, D, [Mg[CH(SiMe3)2]2(OEt2)2], the known [Ce(Cl)[(N(SiMe3)C(Ph))2CH]2] (E) and 16 are reported. The cerium alkyl (like 1) has one close Ce...C contact for each ligand, attributed to a gamma-C-Ce agostic interaction. The Ln alkyls and have a trigonal prismatic arrangement of the chelating ligands (each of the same chirality at Calpha) around the metal. In an arene solution at 313 K exists as two isomers, as evident from detailed NMR spectroscopic experiments.     

Bimetallic-induced tail-to-tail dimerization and C-H activation of methyl acrylate

An organometallic complex resulting from tail-to-tail dimerization and C-H activation of methyl acrylate (MA), [Mo(CO2Cp(eta 3-(MeO2C)CH[symbol: see text]CH[symbol: see text]CHCH2(CO2Me)] 2, has been fully characterized from the reaction of the heterobimetallic complex [Cp*Ni=Mo(mu-CO)(CO)2Cp] with MA and an exclusively eta 3-allyl bonding mode of the coupled ligand was established for the first time by X-ray diffraction; formation of 2 is accompanied by that of the mu 3-alkylidyne-capped cluster [NiMo2(mu 3-CCH2CO2Me)(CO)4Cp*Cp2] 3 which results from a double C-H activation of the CH2 group of MA; none of these reactions occur with the corresponding homodinuclear complexes.