Aluminum carbenoids in allene cyclopropanation

The reactions of aluminum carbenoids with alkyl- and phenyl-substituted allenes and cyclic allenes are studied. An efficient method for the synthesis of substituted spiropentanes was developed. 1,2-Cyclononadiene was selectively converted into bicyclo[7.1.0]dec-1-ene. An unusual transformation of α-methylphenylallene into a spiroindane derivative under the action of Et₃Al-CH₂I₂ was found.     

Migration of a cationic polymer between lipid vesicles

The adsorption of a synthetic polycation, poly(N-ethyl-4-vinylpyridinium bromide) (PEVP), on the surface of bilayer lipid vesicles (liposomes) and the migration of adsorbed macromolecules between the liposomes are studied. Liposomes of three types are used, including (1) traditional two-component liposomes composed of neutral phosphatidylcholine (PC) and anionic cardiolipin (CL); (2) three-component liposomes consisting of PC, CL, and cationic dicetyldimethylammonium bromide (DCMAB); and (3) anionic PC/CL liposomes with a nonionic surfactant, poly(ethylene oxide)-cetyl alcohol ether (Briij 58), incorporated into their bilayers. The adsorption of PEVP on the surface of PC/CL liposomes is accompanied by their aggregation. Using the fluorescence method, it is shown that the units (segments) of the polycation undergo partial redistribution between the liposomes inside the aggregates formed from PC/CL liposomes (with and without a fluorescent label) and PEVP. On the contrary, three-component PC/CL/DCMAB and PC/CL/Briij liposomes are not aggregated, even with the complete neutralization of their charges by adsorbed PEVP. In both cases, the migration of PEVP molecules between individual (nonaggregated) liposomes is observed. Possible reasons for the aggregative stability of the three-component PC/CL/DCMAB and PC/CL/Briij liposomes and the mechanism of interliposome migration of PEVP in such systems are discussed.     

Modulation of interaction of polycations with negative unilamellar lipid vesicles

Interactions of small unilamellar negative vesicles composed of diphosphatidylglycerol (cardiolipin, CL²⁻), 20 mol%, and phosphatidylcholine (egg yolk lecithin, EL), 80 mol%, with various cationic polymers (CP) derived from poly(4-vinylpyridine) (PVP) were studied in water and water–salt solutions by means of photon correlation spectroscopy, microelectrophoresis, conductometry, and fluorescence techniques. The linear charge density and hydrophilic lipophilic balance of CPs were varied by quaternization of PVP with various amounts of different alkyl bromides (ethyl-(2), heptyl-(7), dodecyl-(12), cetyl-(16)). Substantial differences were observed in the behavior of exhaustingly N-ethylated PVP (CP2) and PVP N-ethylated to 50 mol% (CP2(50)) or 30 mol% (CP2(30)). All of them adsorb to the CL²⁻/EL vesicle membrane, neutralizing the surface negative charge and causing aggregation of the vesicles. However, CP2, a polycation with a maximum linear charge density, strongly enhances transfer of the negative lipid ions from the inner to outer bilayer leaflet, while CP2(50) and CP2(30) do not. Adsorbed CP2 does not disturb integrity of the vesicle membrane and can be completely removed from the surface of aggregated vesicles by adding a simple salt (NaCl) or a negative linear polyelectrolyte (polyacrylic acid (PAA) sodium salt). Such removal is followed by release of the original vesicles. In contrast to that, adsorbed CP2(50) or CP2(30) produce some leak through the lipid bilayer and cannot be completely desorbed either by increasing ionic strength or adding an excess of PAA. The probable reason of these differences is discussed. PVP partially N-alkylated with dodecyl or cetyl bromides (3 mol%) and then completely N-ethylated (CP2,12 and CP2,16), also having a maximum linear charge density, adsorbs to the negative vesicle surface as a result of both electrostatic binding and hydrophobic interaction. Bulky hydrocarbon pendant groups incorporate into the inner bilayer compartment. Similarly to CP2(50) and CP2(30), CP2,12 and CP2,16 cannot be removed from the surface either by adding the simple salt, or an excess of PAA. However, in contrast to CP2(50) and CP2(30), the polycations with the bulky hydrocarbon pendant groups do not cause any leak through the vesicle membrane. Finally, we have succeeded to prepare the ternary vesicles also composed of 20 mol% of CL²⁻, but partially replacing EL for polyoxyethylene 20 cetyl ether (Brij 58) (up to 30 mol%). The CL²⁻/EL/Brij vesicle carries a hydrophilic corona formed by polyoxyethylene chains exposed into water, while hydrophobic cetyl radicals are incorporated in the lipid bilayer. The CL²⁻/EL/Brij vesicles adsorb all studied CPs similar to the binary CL²⁻/EL vesicles. This means that polyoxyethylene corona is permeable for polycationic species restricting neither electrostatic binding nor incorporation of bulky hydrocarbon groups of CP2,16 into the membrane. However, the corona effectively stabilizes the CP-vesicle complexes against aggregation when the membrane surface is neutralized.     

Reactions of 1,4-enynes with the system CH2I2-Et3Al

Reactions of alk-1-en-4-ynes with an excess of the system CH₂I₂-Et₃Al give 1-cyclopropylmethyl-1,2-diethylcyclopropanes. A decrease in the amount of either component of the system to two equivalents results in cyclopropanation of the double bond only. Under such conditions, conjugated enynes yield a complex mixture of products, while conjugated diynes are inert to the system CH₂I₂-Et₃Al.     

The reagent Et2AlX/CH2N2 in cyclopropanation of sterically hindered olefins,as well as oxygen- and nitrogen-containing unsaturated compounds

Russian Chemical Bulletin - A transition-metal-free method of cyclopropanation of sterically hindered olefins, substituted allylic alcohols, allylamines, and vinyl silyl ethers was developed using...     

Physicochemical and biological properties of polyampholytes: Quaternized derivatives of poly(4-vinylpyridine)

The modification of poly(4-vinylpyridine) with ω-bromocarboxylic acids and alkyl bromides yields three types of polyampholytes: polyampholytes containing both cationic and anionic groups in each monomer unit (polybetaines), polyampholytes containing betaine and cationic units, and polyampholytes containing betaine units and side cetyl radicals. Their complex formation with liposomes formed from zwitterionic (electroneutral) phosphatidylcholine and anionic diphosphatidylglycerol (cardiolipin) is investigated. The method for fixation of polymers on the liposomal membrane and the stability of the formed complexes are determined by the chemical structure of macromolecules. For the most part, polyelectrolytes are electrostatically adsorbed on the membrane and are fully removed from it with an increase in the salt concentration in the surrounding solution. An exception is the polybetaine obtained through the modification of poly(4-vinylpyridine) with ω-bromobutyric acid, which irreversibly binds to liposomes probably owing to the incorporation of macromolecular fragments into the hydrophobic part of the lipid bilayer. The insertion of side cetyl radicals into polybetaine molecules stabilizes their complexes with liposomes in the presence of salts. The cytotoxicity of the synthesized polyampholytes is one to two orders of magnitude lower than that of a cationic polymer with the same degree of polymerization.     

Aluminum carbenoids in the cyclopropanation of fulvenes

Aluminum carbenoid Et₂AlCH₂I reacts with 6-substituted fulvenes to give tricyclopropanes in high yields. Calculations at the B3LYP/6-31G(d) level of theory show that coplanar arrangement of the double bonds facilitates cyclopropanation due to conjugation in the transition state. Aluminum carbenoid Et₂AlCH₂I was generated by either the reaction of equimolar amounts of Et₃Al and CH₂I₂ in hexane or treatment of Et₂AlI with CH₂N₂ in dichloromethane.     

What is the effective charge of TGA-stabilized CdTe nanocolloids?

The surface charge of semiconductor nanoparticles, Q, is an important parameter which determines their electrokinetic behavior, stability in water and polar solvents, functions of optical and electronic devices, self-assembly properties, and interactions with cell membranes. We have developed a simple method for quantitative determination of Q in their native aqueous environment. The method does not require the knowledge of exact atomic structure or make assumptions about effects of drying on charge distribution. The method is based on titration of nanoparticle dispersion with a solution of oppositely charged polyelectrolyte. The point of complete neutralization is recognized as an inflection point on the dependence of fluorescence intensity on the amount of polyelectrolyte added. Thioglycolic acid-stabilized CdTe nanoparticles 2 nm in diameter were found to carry an average Q from -2.6 to -5.5 for pH 7.5 to 10, respectively. This charge is found to be smaller than that calculated theoretically for an analogous structure (i.e., Q = -8), presumably due to adsorption of Cd(2+) ions on the stabilizer shell and on Te atoms with unsaturated valence located on the side planes of CdTe tetrahedrons.     

Polyelectrolyte-coated liposomes: stabilization of the interfacial complexes

Anionic liposomes, composed of egg lecithin (EL) or dipalmitoylphosphatidylcholine (DPPC) with 20 mol% of cardiolipin (CL(2-)), were mixed with cationic polymers, poly(4-vinylpyridine) fully quaternized with ethyl bromide (P2) or poly-l-lysine (PL). Polymer/liposome binding studies were carried out using electrophoretic mobility (EPM), fluorescence, and conductometry as the main analytical tools. Binding was also examined in the presence of added salt and polyacrylic acid (PAA). The following generalizations arose from the experiments: (a) Binding of P2 and PL to small EL/CL(2-) liposomes (60-80 nm in diameter) is electrostatic in nature and completely reversed by addition of salt or PAA. (b) Binding can be enhanced by hydrophobization of the polymer with cetyl groups. (c) Binding can also be enhanced by changing the phase state of the lipid bilayer from liquid to solid (i.e. going from EL to DPPC) or by increasing the size of the liposomes (i.e. going from 60-80 to 300 nm). By far the most promising systems, from the point of view of constructing polyelectrolyte multilayers on liposome cores without disruption of liposome integrity, involve small, liquid, anionic liposomes coated initially with polycations carrying pendant alkyl groups.