Anion-receptor molecules: Macrocyclic and macrobicyclic effects on anion binding by polyammonium receptor molecules

The stability constants for anion binding by the acyclic hexaamine 1 , its macrocyclic analogue 2 , and the bicyclic compound 3 in their protonated forms are reported. Compound 3 forms stable and selective complexes with halide ions, the stability sequence being I^? > Br^? > Cl^?. Compound 2 forms more stable complexes with sulfate, oxalate, and malonate dianions than its acyclic analogue 1 and shows a better selectivity pattern. Compound 3 forms stronger complexes with oxalate^2? than 2 and shows a remarkably high binding selectivity between oxalate^2? and malonate^2?. The comparison of the ability of 1–3 to complex anions demonstrates the macrocyclic and macrobicyclic effects on anion binding stability and selectivity.     

Quantum-chemical investigation of the mechanism of the reaction of six-membered cyclic boronic esters with acetonitrile

Determination of the energ of the intermediate ions in the reaction of 1,3,2-dioxa- and oxazaborinanes with acetonitrile by the AM1 method showed that the yield of the desired 5,6-dihydro-1,3-oxazines under the conditions of thermodynamic control is determined by the relative stability of the carbocation at the stage preceding the addition of the acetonitrile molecule. A. V. Bogatskii Physical Chemistry Institute, National Academy of Sciences of Ukraine, 86 Lustdorfskaya Doroga, Odessa 65080, Ukraine. Translated from Teoreticheskaya i éksperimental'naya Khimiya, Vol. 36, No. 3, pp. 159–161, May–June, 2000.     

Zr-Mediated hydroboration: stereoselective synthesis of vinyl boronic esters

An improved process for the preparation of (E)-vinylboronic esters via a Zr-mediated hydroboration of alkynes, especially oxygen-containing alkynes, is described.     

Coumarin-strapped calix[4]pyrrole: a fluorogenic anion receptor modulated by cation and anion binding

A new strapped calix[4]pyrrole containing a fluorophore as part of the strap has been synthesized and characterized. Association constants with various anions have been determined using both fluorescence titration and isothermal titrations calorimetry (ITC). The two sets of association constants were found to be in good agreement with one another. The fluorescence emission properties of this new receptor could be controlled by addition of Na+ (or H2O) and anions. However, the fluorescence quenching by anions is only observed in the presence of Na+ (or H2O). All the experimental evidence is consistent with the notion that independent PET processes are modulated by separate cation and anion recognition events. As such, this system operates as an elementary logic gate wherein anion and cation concentrations serve as the input and fluorescence intensity changes provide the output.     

Synthesis and carboxylate anion binding studies on cyclic sugar-amino acid hybrids

Abstract

Here in, the condensation of boc-glycine with 2,6-anhydro-3,4,5-tri-O-benzyl-D-gluco-heptitol followed by its boc-deprotection to form 2,6-anhydro-3,4,5-tri-O-benzyl-D-gluco-heptitolyl bis-glycinate, which in turn on condensation with succinic acid/pyridine-2,6-dicarboxylic acid led to the formation of sugar-amino acid hybrid macrocyclic compounds 4, 6 and debenzylated marocyclic compound 5, having amide bonds that function as efficient host for polar, hydrogen bond acceptors and carboxylate ions. The anion inclusion capability of synthesized macrocylic hosts has been evaluated by the study of their binding with boc-GlyCOOˉ anion as guest through 1H NMR titration studies in CDCl₃. The binding constant (K_a) of boc-GlyCOOˉ guest with macrocyclic hosts 4 and 6 involving succinate and pyridine-2,6-dicarboxylate linkers was found to be 9.201?×?10³ and 1.437?×?10⁴ M^?1, respectively. The higher binding constant was observed in the complex of boc-GlyCOOˉ with pyridine-dicarboxylate containing host may be due to the extra rigidity & suitable conformation attained by the presence of rigid-aromatic dicarboxylate linker.     

An electrophilic cleavage procedure for the asymmetric dihydroxylation: direct enantioselective synthesis of cyclic boronic esters from olefins

A variation within the osmium-catalysed asymmetric dihydroxylation (AD) of olefins is described that yields cyclic boronic esters from olefins in a straight-forward manner. This process represents the first real product alteration in asymmetric dihydroxylation, since all previous protocols lead to free diols exclusively. A protocol based on the Sharpless AD conditions (for enantioselective oxidation of prochiral olefins) was developed that gives cyclic boronic esters with excellent enantiomeric excesses (ee's). Some of the ee's are higher than those reported for conventional AD. The unprecedented role of phenyl boronic acid on the course of the AD reaction was investigated in detail. PhB(OH)2 does not interfere with the chiral ligand, leaving the enantioselective step of olefin oxidation intact. The main role of the boronic acids-apart from protecting the diol products against potential overoxidation-relies on removing the diol entity in an electrophilic cleavage, which is in contrast to the conventional hydrolytic cleavage of the AD protocols. Thus, a mechanistically new cleavage for enantioselective dihydroxylation reactions is introduced within the present work.     

Analysis of 1,2-diols of linoleic, alpha-linolenic and arachidonic acid by gas chromatography--mass spectrometry using cyclic alkyl boronic esters

Arachidonic acid is metabolized by hepatic and renal cortical microsomes in the presence of NADPH to vicinal dihydroxyeicosatrienoic acids as some of the major metabolites. Other polyunsaturated, long-chain fatty acids might be metabolized to vicinal dihydroxy acids (1,2-diols) in the same way. To facilitate identification of 1,2-diols in biological samples, a series of unsaturated 1,2-diols were synthesized from linoleic, alpha-linolenic and arachidonic acid and the electron-ionization mass spectra of cyclic methane- and n-butaneboronic ester derivatives and of trimethylsilyl (TMS) ether derivatives were compared. The TMS ether derivatives gave rise to weak molecular ions but prominent informative fragmentation ions were formed by alpha-cleavage as well as cleavage between the carbons with the TMS ethers. The TMS ether derivative of methyl 15,16-dihydroxy-9,12-octadecadienoate had a considerably larger carbon value than the other C18 diols, while the cyclic boronates were poorly separated on gas chromatography. The methane- and n-butaneboronic acid derivatives showed strong molecular ions and a characteristic but not very informative fragmentation, although the position of the hydroxyls could be deduced from one or two fragments formed by alpha-cleavage. Linoleic and alpha-linolenic acid are metabolized in the rabbit to many polar products by hepatic and renal cortical microsomes and NADPH. 12,13-Dihydroxy-9-octadecenoic acid and other metabolites of linoleic acid were identified by gas chromatography--mass spectrometry.     

Reagent-controlled asymmetric homologation of boronic esters by enantioenriched main-group chiral carbenoids

[reaction: see text] Putative enantioenriched carbenoid species, (R)-1-chloro-2-phenylethylmagnesium chloride (9) and (S)-1-chloro-2-phenylethyllithium (26), generated in situ by sulfoxide ligand exchange from (-)-(R(S),R)-1-chloro-2-phenylethyl p-tolyl sulfoxide (8), effected the stereocontrolled homologation of boronic esters. sec-Alcohols derived from the product boronates by oxidation with basic hydrogen peroxide exhibited % ee closely approaching that of sulfoxide 8 in examples employing Li-carbenoid 26.     

Selective recognition of pyrophosphate in water using a backbone modified cyclic peptide receptor

A cyclic peptide based receptor, bearing two dipicolylamino arms complexed to zinc(II) ions, binds pyrophosphate ions with high affinity and selectivity in aqueous solution as determined using an indicator displacement assay.     

Synthesis of hindered anilines: copper-catalyzed electrophilic amination of aryl boronic esters

No longer a hindrance: copper-catalyzed electrophilic amination of aryl boronic esters is accomplished under mild reaction conditions using 2.5-5.0 mol % of a catalyst derived from copper tert-butoxide and Xantphos ligand. The reaction tolerates a wide range of functional groups and can be used to prepare some of the most hindered anilines made to date.     

Controlled polymerization of activated glycine esters by copper(II) chelate

We describe a novel method of polymerization, via the insertion of activated glycine esters into N‐salicylideneglycinato‐aquo‐copper(II) chelate ( 1 ), that uses the reactivity of the metal chelate. In the absence of 1 , a high molecular weight polyglycine was formed as a white precipitate after triethylamine was added to an N,N‐dimethylformamide solution of 4‐nitrophenyl glycinate ( 3a ). In the presence of 5 mol % 1 , however, the polymerization proceeded homogeneously. After the reaction mixture was poured into tetrahydrofuran, a condensation product of glycine was obtained. According to gel permeation chromatography analysis, the product consisted of high and low molecular weight fractions. The former and latter were obtained by self‐polycondensation and polycondensation via the insertion of 3a into 1 , respectively. So that the self‐polycondensation of activated glycinates would be depressed, 2‐chlorophenyl ( 3b ), 3‐chlorophenyl ( 3c ), 4‐chlorophenyl, and phenyl glycinates were used as less activated glycine esters. For the polymerization of 3b and 3c , the polymerization via the insertion of activated glycinates into 1 was promoted. © 2003 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 41: 1504–1510, 2003     

Metal-free synthesis of aryl esters by coupling aryl carboxylic acids and aryl boronic acids

A facile synthesis of aryl esters is developed by coupling aryl carboxylic acids and aryl boronic acids in the presence of PhI(OAc)₂ and carbonyl diimidazole. A wide range of functional groups were tolerant to the metal-free reaction condition that led to the desired products in good yields.     

Thermoplasticization of cellulose acetates by grafting of cyclic esters

A plasticization method for cellulose acetates (CAs) based on the selective grafting of caprolactone (CL) and L-lactide (LACD) has been developed. The selectivegrafted products could be prepared by ring opening polymerization in the melt state at 140°C using stannous octoate as catalyst, where CAs with remaining hydroxyl groups worked as initiator. Plasticization of CAs by this selective grafting can solve the problem encountered in the previous reports (Yoshioka et al., 1996, 1998) that the bleeding of unreacted monomers and homooligomers from the inside of molded articles to their surface was often found. By using adequate reaction conditions, the grafting reaction proceeded rapidly and could be completed within 10–30min. LACD is grafted more rapidly than CL onto CAs, producing relatively rigid and brittle products in the earlier stages and elastomerlike ones in the later stages. Transparent amorphous molded articles were obtainable depending on the reaction conditions. The analysis of the structure of the grafted side chains by means of high resolution NMR spectroscopy showed that, although the grafted side chains are composed of large amounts of oxycaproyl or lactidyl block polymer portions depending on the reaction conditions, a large amount of randomly polymerized parts coexist in the grafted chains, which confer high thermoplasticity, elasticity and amorphous nature to the grafted products obtained.     

Epoxide formation by the photolysis of cyclic oxalate esters

The cyclic oxalate esters from $\text{meso}$- and $\text{d}$, $\text{1}$-hydrobenzoin were prepared and photolyzed. $\text{Meso}$-hydrobenzoin oxalate gave only $\text{cis}$-stilbene oxide upon photolysis while the $\text{d}$, $\text{1}$ isomer gave $\text{trans}$-stilbene oxide.     

Intestinal permeability of cyclic peptides: common key backbone motifs identified

Insufficient oral bioavailability is considered as a key limitation for the widespread development of peptides as therapeutics. While the oral bioavailability of small organic compounds is often estimated from simple rules, similar rules do not apply to peptides, and even the high oral bioavailability that is described for a small number of peptides is not well understood. Here we present two highly Caco-2 permeable template structures based on a library of 54 cyclo(-D-Ala-Ala(5)-) peptides with different N-methylation patterns. The first (all-trans) template structure possesses two β-turns of type II along Ala(6)-D-Ala(1) and Ala(3)-Ala(4) and is only found for one peptide with two N-methyl groups at D-Ala(1) and Ala(6) [(NMe(1,6)]. The second (single-cis) template possesses a characteristic cis peptide bond preceding Ala(5), which results in type VI β-turn geometry along Ala(4)-Ala(5). Although the second template structure is found in seven peptides carrying N-methyl groups on Ala(5), high Caco-2 permeability is only found for a subgroup of two of them [NMe(1,5) and NMe(1,2,4,5)], suggesting that N-methylation of D-Ala(1) is a prerequisite for high permeability of the second template structure. The structural similarity of the second template structure with the orally bioavailable somatostatin analog cyclo(-Pro-Phe-NMe-D-Trp-NMe-Lys-Thr-NMe-Phe-), and the striking resemblance with both β-turns of the orally bioavailable peptide cyclosporine A, suggests that the introduction of bioactive sequences on the highly Caco-2 permeable templates may result in potent orally bioavailable drug candidates.