Room-temperature polycondensation of β-amino acid derivatives VI. Synthesis of various N-(hydroxyethyl) nylons

Various N-(hydroxyethyl)amino acid esters having a methyl substituent or phenyl group between amine and ester groups have been synthesized and their polycondensation behavior was investigated. These substituted amino acid esters gave amorphous polyamides which were soluble in alcohol. A model reaction between N-(hydroxyethyl)-amine and carboxylic acid ester was carried out in order to elucidate the role of hydroxyethyl group on the polycondensation. It was found that the amidation reaction took place rapidly at room temperature when the alkyl group of the carboxylic acid was small. N-(Hydroxyethyl) polyamides were obtained from N,N′-(bishydroxyethyl)-dicamines and dicarboxylic acid esters. The reaction mechanism of the room-temperature polycondensation reaction is discussed.     

Room-temperature polycondensation of β-amino acid derivatives,I. Polyamide from amino alcohols and acrylates

Acrylates, such as ethyl acrylate, add with amino alcohol to form N-(hydroxyalkyl) β-alanine ester and room-temperature polycondensation follows, forming polyamide in the presence of a basic catalysts, such as alkali metal alkoxide. The reaction medium has an influence on the course of the polycondensation; that is, N-(hydroxyalkyl) polyamide is formed in methanol solution and polyamide ether in other solvents, such as tetrahydrofuran. These two courses of the room-temperature polycondensation have been studied, and the reaction mechanism is discussed in this paper.     

The synthesis of β-heteroarylamino-α,β-dehydro-α-amino acid and β-heteroarylamino-α-amino acid derivatives

From heteroarylaminomethyleneoxazolones 4 , obtained from N-heteroarylformamidines 2 and 2-phenyl-5-oxo-4,5-dihydro-1,3-oxazole ( 3 ), the following β-heteroarylamino-α,β-dehydro-α-amino acid derivatives were prepared: methyl 8 and ethyl esters 9 , amides 10 and 11 , hydrazides 12 , and azides 15 . By catalytic hydrogenation the compounds 4 were converted into β-heteroarylamino substituted amides 18 and β-heteroarylamino-α-amino acids 20 .     

Poly(β-amino acid)s. IV. Synthesis and conformational properties of poly(α-isobutyl-L-aspartate)

Poly(α-isobutyl-L -aspartate) was prepared by the polycondensation reaction of p-nitrophenyl ester of α-isobutyl-L -aspartate and the conformation of the poly(β-amino acid) was investigated by X-ray diffraction, polarized infrared, circular dichroism (CD), optical rotatory dispersion (ORD), and NMR spectroscopy. α-Isobutyl β-p-nitrophenyl-L -aspartate hydrochloride and hydrobromide were used as monomers and dimethylformamide, chloroform, and chlorobenzene, as solvents. A high-molecular-weight polymer with [η] 1.0 dl/g (dichloroacetic acid, 25°C) was formed in the polymerization of the hydrochloride in chloroform at 25°C. The X-ray diagram and polarized infrared spectrum of the stretched polymer film obtained from a chloroform solution suggested a cross-β-form as the most probable structure in the solid state. The CD spectra of the polymer in a 2,2,2-trifluoroethanol (TFE) solution and its film cast from the solution showed a peak at 205 nm and a trough at 190 nm which were assigned to a β-structure. The polymer was associated in chloroform. The NMR and ORD spectra in chloroform were similar to those in TFE, which suggests that the polymer also exists in the β-structure in chloroform. The addition of small amounts of dichloroacetic acid and sulfuric acid to chloroform and TFE solutions, respectively, destroyed the β-structure. A random copolymer of α-isobutyl-L -aspartate with β-alanine was also prepared by polycondensation reaction. The copolymer apparently did not form an ordered structure in the solid state or in solution.     

Poly(β-Amino acids). VI. Synthesis and conformational properties of poly[(r)-3-pyrrolidinecarboxylic acid]

Racemic and optically active 3-pyrrolidinecarboxylic acids (β-proline) were synthesized, and their polymers, poly[(RS)-β-proline] and poly[(R)-β-proline], were prepared by the polycondensation reaction of the p-nitrophenyl esters. Model compounds, N-cyclopentylcarboxylic acid pyrrolidide and N-cyclopentylcarbonyl-(R)-3-pyrrolidinecarboxylic acid pyrrolidide, were synthesized to elucidate the conformation of the polymer. The solution properties of poly[(R)-β-proline] and the model compounds were investigated by means of circular dichroism (CD) and NMR spectroscopy. The spectral patterns of the polymer and model compounds were similar in various solvents. Poly[(R)-β-proline] and poly[(RS)-β-proline] showed identical NMR spectra. These results suggest that poly[(R)-β-proline] may exist in a random conformation consisting of mixtures of cis and trans amide bonds. The conformational study of cyclopentanecarboxylic acid pyrrolidide by NMR spectroscopy with a shift reagent, Eu(fod)₃, in CDCl₃ implied that the plane containing the amide group bisects the cyclopentane ring. This suggests that each amide plane in the polymer in chloroform may also bisect the pyrrolidine ring.     

Chemical synthesis of poly‐γ‐glutamic acid by polycondensation of γ‐glutamic acid dimer: Synthesis and reaction of poly‐γ‐glutamic acid methyl ester

α‐Methyl glutamic acid (L ‐L )‐, (L ‐D )‐, (D ‐L )‐, and (D ‐D )‐γ‐dimers were synthesized from L ‐ and D ‐glutamic acids, and the obtained dimers were subjected to polycondensation with 1‐(3‐dimethylaminopropyl)‐3‐ethylcarbodiimide hydrochloride and 1‐hydroxybenzotriazole hydrate as condensation reagents. Poly‐γ‐glutamic acid (γ‐PGA) methyl ester with the number‐average molecular weights of 5000∼20,000 were obtained by polycondensation in N,N‐dimethylformamide in 44∼91% yields. The polycondensation of (L ‐L )‐ and (D ‐D )‐dimers afforded the polymers with much larger |[α]_D | compared with the corresponding dimers. The polymer could be transformed into γ‐PGA by alkaline hydrolysis or transesterification into α‐benzyl ester followed by hydrogenation. © 2001 John Wiley & Sons, Inc. J Polym Sci A: Polym Chem 39: 732–741, 2001     

Short synthesis of tryptophane and β-carboline derivatives by reaction of indoles with N-(diphenylmethylene)-α,β-didehydroamino acid esters

The ethylaluminum dichloride catalyzed Michael-type addition of indoles 1a-h to the N-(diphenylmethylene)-α,β-didehydroamino acid esters 2a-c allows a new synthesis of β-methyltryptophanes 41,m and a new route for 1,1-diphenyl-3-carbalkoxy-1,2,3,4-tetrahydro-β-carbolines 5a-m.     

Unprecedented polymerization of δ‐valerolactone initiated by the stable enolate of γ‐butyrolactone

Polymerization of δ‐valerolactone has been studied using γ‐butyrolactone enolate as initiator. Mechanistic studies show that the initiation proceeds with incorporation of the initiator into the growing polymer chain and acyl‐oxygen bond cleavage of the monomer. The molecular weight distribution of the resulting polymers is narrow compared to that of poly(δ‐valerolactone) obtained from common anionic initiators, e. g. alkali metal alkoxides.     

Multichain copoly(α-amino acid). III. Multichain copoly(α-amino acid) prepared by the reaction of copoly(L-lysine γ-methyl-L-glutamate) with N-carboxy anhydride of β-benzyl L-aspartate

Graft copolymerization of N-carboxy anhydride of β-benzyl-L -aspartate onto copoly(L -lysine γ-methyl-L -glutamate) was carried out in N,N-dimethylformaide which contained 3 v/v% of dimethyl sulfoxide to obtain multi-N^ε-poly(β-benzyl-L -aspartyl)copoly(L -lysine γ-methyl-L gluta mate). The degree of polymerization of the branch chain attained was much influenced by the interval of the grafting sites of the copoly(L -lysine γ-methyl-L -glutamate). The solvent-induced two-step conformational transition of the multichain copoly(α-amino acid) was observed in the chloroform-dichloroacetic acid system at 25°C by the ORD technique. The stability of the α-helical conformation of the backbone polymer chain was decreased by the presence of poly(β-benzyl-L -aspartyl) branch chains that could form unstable α-helical conformations of opposite spirals.     

β-Carbolines as agonistic or antagonistic benzodiazepine receptor ligands. 1. Synthesis of some 5-, 6- and 7-amino derivatives of 3-methoxycarbonyl-β-carboline (β-CCM) and of 3-ethoxycarbonyl-β-carboline (β-CCE)

Condensation of diethyl formylamino- or diethyl acetylaminomalonate with 4-, 5- or 6-nitrogramine 1 afforded the diethyl formylamino- or the diethyl acetylamino[(nitroindol)-3-ylmethyl]malonates 2 ; reduction of the nitro group followed by N-formylation or acetylation of the resulting amino compounds 3 , led to the 4-, 5-and 6-acylamino derivatives 4 . Cyclization of 4 in the presence of polyphosphoric esters gave the 3,3-bis(ethoxycarbonyl)-3,4-dihydro-β-carbolines 5 , which underwent lithium chloride/water catalyzed monodeethoxycarbonylation to the corresponding 5-, 6- and 7-acylamino-3-ethoxycarbonyl-β-carbolines 6 , whose acidic hydrolysis led finally to the 5-, 6- and 7-amino-3-ethoxycarbonyl-β-carbolines 9 . The 6-amino compounds 9b-e were obtained also by direct nitration of 3-methoxycarbonyl-β-carboline 7a and of 3-ethoxycarbonyl-β-carboline 7c , followed by the nitro group reduction of the resulting nitro carbolines 8 . Preliminary studies of the binding to rabbit brain benzodiazepine receptor sites indicate compounds 9b and 9c to inhibit the ³H-diazepam binding at 10^?8 M concentrations.     

High-molecular-weight poly(amino acid)s by the direct polycondensation reaction promoted by triphenyl phosphite and LiCl in the presence of polyvinylpyrrolidone

Poly(α-amino acid)s of high molecular weight were obtained by the direct polycondensation reaction of α-amino acids in the presence of polyvinylpyrrolidone (PVP) as a matrix of triphenyl phosphite and LiCl in N-methylpyrrolidone (NMP). Molecular weights of the polymer produced were improved by use of an increasing amount of matrix of higher molecular weight. Most favorable results were obtained by the reaction at 80°C for 16 hr at a monomer concentration of 0.33 mole/liter in a NMP solution that contained about 3 wt % LiCl in the presence of an equivalent unit mole of PVP with the molecular weight of 3.6 x 10⁵. The polymer from β-alanine with high molecular weight, which is difficult to obtain by the NCA method, was easily prepared by this process.     

Polymerization of α-amino acid N-carboxy anhydrides. III. Mechanism of polymerization of L- and DL-alanine NCA in acetonitrile

The polymerization of L - and DL -alanine NCA initiated with n-butylamine was carried out in acetonitrile which is a nonsolvent for polypeptide. The initiation reaction was completed within 60 min.; there was about 10% of conversion of monomer. The number-average degree of polymerization of the polymer obtained increased with the reaction period, and it was found to agree with value of W/I, where W is the weight of the monomer consumed by the polymerization and I is the weight of the initiator used. The initiation reaction of the polymerization was concluded as an attack of n-butylamine on the C₅ carbonyl carbon of NCA. The initiation, was followed by a propagation reaction, in which there was attack by an amino endgroup of the polymer on the C₅ carbonyl carbon of NCA. The rate of polymerization was observed by measuring the CO₂ evolved, and the activation energy was estimated as follows: 6.66 kcal./mole above 30°C. and 1.83 kcal./mole below 30°C. for L -alanine NCA; 15.43 kcal./mole above 30°C., 2.77 kcal./mole below 30°C. for DL -alanine NCA. The activation entropy was about ?43 cal./mole-°K. above 30°C. and ?59 cal./mole-°K. below 30°C. for L -alanine NCA; it was about ?14 cal./mole-°K. above 30°C. and ?56 cal./mole-°K. below 30°C. for DL -alanine NCA. From the polymerization parameters, x-ray diffraction diagrams, infrared spectra, and solubility in water of the polymer, the poly-DL -alanine obtained here at a low temperature was assumed to have a block copolymer structure rather than being a random copolymer of D - and L -alanine.     

Effect of chelation on the polycondensation of monomers having an active ester group

Various amino acid esters and dicarboxylic acid esters having a β-thioether group have been synthesized and their polycondensation with diamine was found to occur at room temperature to form polyamide thioether. The effect of solvents or chelating agents on their polycondensation reaction was investigated. Metal acetylacetonates or inorganic salts had a great influence on the rate of the polycondensation reaction, and the catalytic activity of metal acetylacetonates M(AcAc)_n or inorganic salts decreased in the following order: Mg(AcAc)₂?Th(AcAc)₄>Cu(AcAc)₂>Li(AcAc)>None>Zr(AcAc)₄, MgCl₂·6H₂O>CuCl₂·.2H₂O>ZnCl₂>MgCl₂>None. It was also found that the amount of polyamide thioether was dependent on solvents or the presence of chelating agents because the polycondensation rate and the apparent equilibrium between ring and chain structures were both greatly influenced by solvents or chelating agents. These effects of solvents or chelating agent on the polycondensation may be attributable to formation of a complex with the thioether group which enhances the reactivity of ester.     

Transformations of N-heteroarylformamidines into derivatives of β-heteroarylamino-α,β-dehydro-α-amino acids, β-heteroarylamino-α-amino acids,and dipeptides

Transformations of N'-heteroaryl-N,N-dimethylformamidines 1 as a general method for the preparation of β-heteroarylamino-α,β-dehydro-α-amino acids, β-heteroarylamino-α-amino acid derivatives 5–9 , and dipeptides 10 , are described.     

Linear,Peptidase‐Resistant β2/β3‐Di‐ and α/β3‐Tetrapeptide Derivatives with Nanomolar Affinities to a Human Somatostatin Receptor,Preliminary Communication

N‐Acyl‐β²/β³‐dipeptide‐amide somatostatin analogs, 5 – 8 , with β²‐HTrp‐β³‐HLys ('natural' sequence) and β²‐HLys‐β³‐HTrp (retro‐sequence) have been synthesized (in solution). Depending on their relative configurations and on the nature of the terminal N‐acyl and terminal C‐amino group, the linear β‐dipeptide derivatives have affinities for the human receptor hsst 4, ranging from 250 to >10000 nanomolar (Fig. 3). Also, N‐Ac‐tetrapeptide amides 9 and 10 , which contain one α‐ and three β‐amino acid residues (N‐β‐α‐β‐β‐C), have been prepared (solid‐phase synthesis), with the natural (Phe, Trp, Lys, Thr) and the retro‐sequence (Thr, Lys, Trp, Phe) of side chains and with two different configurations, each, of the two central amino acid residues. The novel ‘mixed', linear α/β‐peptides have affinities for the hsst 4 receptor ranging from 23 to >10000 nanomolar (Fig. 4), and, like ‘pure' β‐peptides, they are completely stable to a series of proteolytic enzymes. Thus, the peptidic turn of the cyclic tetradecapeptide somatostatin (Fig. 1) can be mimicked by simple linear di‐ and tetrapeptides. The tendency of β‐dipeptides for forming hydrogen‐bonded rings is confirmed by calculations at the B3LYP/6‐31G(d,p) level (Fig. 2). The reported results open new avenues for the design of low‐molecular‐weight peptidic drugs.     

β-Cleavage of Bis(homoallylic) Potassium Alkoxides. Two-Step Preparation of Propenyl Ketones from Carboxylic Esters. Synthesis of ar-Turmerone, α-Damascone, β-Damascone,and β-Damascenone

The transformation of 36 bis(homoallylic) alcohols VII to alkenones IX and X via β-cleavage of their potassium alkoxides VIIa in HMPA has been investigated (cf. Scheme 2). These studies have established an order of β-cleavage for 2-propenyl, 1-methyl-2propenyl, 2-methyl-2-propenyl, 1,1-dimethyl-2propenyl, and benzyl groups in alkoxides 49a – 56a and have allowed a comparison between the β-cleavege reaction and the oxy-Cope rearrangement in alkoxides 74a – 83a . As illustrative syntheti applications, a two-step preparatio of propenyl ketones 15 – 42 from carboxylic esters is described, together with syntheses of ar-turmerone ( 48 ), α-damascone ((E)- 71 ), β-damascone ((E)- 109 ), and β-damascenone ((E)- 111 ).     

Multichain copoly(α-amino acid). I. Multichain copoly(α-amino acid) prepared by reaction of copoly(L-lysine γ-methyl-L-glutamate) with N-carboxy anhydride of Nϵ-carbobenzyloxy-L-lysine

Polymerization of the N-carboxy anhydride of N^?-carbobenzyloxy-L -lysine in the presence of multifunctional polymeric initiator, copoly(L -lysine γ-methyl-L -glutamate) was studied in N,N-dimethylformamide containing 3% (v/v) of dimethyl sulfoxide. Multichain copoly(α-amino acid), i.e., multi-N^?-poly(N^?-carbobenzyloxy-L -lysine)copoly(L -lysine γ-methyl-L -glutamate), was obtained with linear poly(N^?-carbobenzyloxy-L -lysine) as by-product that could be removed by reprecipitation as was evidenced by gel-permeation chromatography. The degree of polymerization of the branch polymer chains estimated by the osmometric molecular weight determination and amino acid analysis was between 20 and 60, which decreased with increasing lysine content of the polymeric initiator. The stability of α-helical conformation of the multichain copoly(α-amino acid) was studied in the chloroform–dichloroacetic acid system at 25°C by the ORD technique. The α-helical conformation of poly(N^?-carbobenzyloxy-L -lysine) branches was less stable than those of linear poly(N^?-carbobenzyloxy-L -lysine) and the core molecular chains of the multichain copoly(α-amino acid).     

Thiophenoanthracene-based conjugated polymers via direct arylation polycondensation

3,4-Appended thiophene monomers furnish unique optoelectronic properties due to electronic and steric effects on the donor unit. Here, we have demonstrated a new polymer synthesis by direct arylation polycondensation of 9,10-dihydro-9,10-[3,4]thiophenoanthracene, a thiophene-based monomer. Chloride-promoted direct arylation polycondensation of 9,10-dihydro-9,10-[3,4]thiophenoanthracene with dibromo monomers with acetate in N,N-dimethylacetamide gave conjugated alternating copolymers. The obtained polymer had a molecular weight of 38,000 and exhibited high film-forming ability. The optical and electrochemical properties of the polymers were also discussed.     

Some properties of poly-α-piperidone

The high molecular weight polymer of α-piperidone, which had been unobtainable with the use of alkali metal, trialkyl aluminum, or Grignard reagent as catalyst, was prepared with M–AlEt₃, (where M is alkali metal), MAlEt₄ or KAlEt₃ (piperidone) as catalyst and N-acyl-α-piperidone as initiator. From the determination of the behavior of the solution viscosity of poly-α-piperidone in m-cresol at 30°C. the value of 0.27 for the Huggins constant was obtained. Examination of the correlation between the number-average molecular weight, determined by endgroup titration, and the intrinsic viscosity gave a somewhat small value for the endgroup COOH. This may be considered due to the consumption of N-acyl-α-piperidone by a propagating polymer in the course of polymerization. The thermal stabilities of the polyamides, nylons 4, 5, and 6, was in the order nylons 6 > 5 > 4 according to differential thermal and thermogravimetric analyses, Poly-α-piperidone, which has a reduced viscosity of 0.7, shows a melting point of 270°C.. which was expected from the zigzag pattern of the correlation between melting points and numbers of CH₂ groups for polyamino-acid polymers.     

Regioselective ring-opening anionic polymerization of β-lactones

New aspects of anionic polymerization of 4-membered lactones are presented, attention being paid to regioselectivity of ß-lactones ring-opening reactions. It has been demonstrated that supramolecular complexes of alkali metal alkoxides used as initiators enable control of lactones polymerization, and due to anion activation yield polymers with specific molecular architecture. Synthesis of the analogue of natural polymer poly(3-hydroxybutyrate) via anionic polymerization of ß-butyrolactone is discussed.