Thermodynamic and structural insight into the underlying mechanisms of the phosphatidylcholine liposomes - casein associates co-assembly and functionality.

The combination of data obtained from isothermal mixing calorimetry and light scattering allowed us to reveal the relationships between the character of the interactions of casein (ß-casein and sodium caseinate (SCN) particles) with phosphatidylcholine (PC) liposomes and their specific properties, such as, the hydrophilic-lipophilic balance of the surface properties, the size, and the architecture. The size distribution diagrams, obtained by dynamic light scattering for the particles of pure PC, ß-casein and their complexes, indicated the involvement of both the protein and liposome particles in the complex formation at pH 5.5 and low ionic strength (0.001 M). As this took place, the data of the extraction of the free PC from the aqueous solutions of the complex particles by diethyl ether showed about 90% of the binding of the PC liposomes by the ß-casein particles. As a result of the interactions, the complex particles showed markedly higher values of their density, calculated on the basis of the light scattering data, as compared to the ones, which were inherent to the pure protein particles. The generality of the importance of such a structural parameter as the density of the complex (protein + PC) particles for their function as protectors against oxidation for the unsaturated PC was supported by the data obtained for the complex particles formed between SCN and PC liposomes at pH 5.5, 40 °C and the low ionic strength (0.001 M). In addition, the importance of both the density and the architecture of the complex (protein + PC) particles for their susceptibility to the proteolysis in the gastrointestinal tract was illustrated by the example of the proteolysis of the complex (ß-casein + PC) particles in the simulated gastrointestinal conditions in vitro.

[The structure and antiviral activity of ribavirin analogs. I. Molecular and crystal structure of 1-(2-hydroxyethoxymethyl)-1,2,4-triazole-5-carboxamide]. / Struktura i protivovirusnaia aktivnost' analogov ribavirina. I. Molekuliarnaia i kristallicheskaia struktura 1-(2-gidroksiétoksimetil)-1,2,4-triazol-5-karboksamida.

The crystal and molecular structures of the antiviral compound 1-(2-hydroxyethoxymethyl)-1,2,4-triazole-5-carboxamide has been determined by the X-ray diffraction method. The space group is P2i/c, unit cell parameters a = 4,381, b = 18,679, c = 10,776 A, beta = 107,40 degrees, Z = 4. The structure was solved by the direct method and refined by a full-matrix least-squares procedure to R = 4.9%. Two planar groups of atoms can be distinguished in the molecule. The first group involves the atoms of triazole ring, C6, and C1', the second one contains C5, C6, O6 and N6 atoms. The angle between these planes is 5.6 degrees. The carboxyamide group is rotated by 180 degrees in comparison with this group in ribavirin. That is why the intramolecular hydrogen bond C1'-H1'. 1...O6 can form. Torsion angle O5'-C5'-C4'-O4' is 73.9 degrees and it corresponds to gauche-rotamer. The conformation about O4'-C4' bond is trans. The C1'-C4' bond is approximately perpendicular to the aglycone.

[The structure and antiviral activity of ribavirin analogs. III. Molecular and crystal structure of 1-(2-hydroxyethoxymethyl)-1,2,4-triazole-carboxamide]. / Struktura i protivovirusnaia aktivnost' analogov ribavirina. III. Molekuliarnaia i kristallicheskaia struktura 1-(2-gidroksiétoksimetil)-1,2,4-triazol-3-karboksamida.

The crystal and molecular structure of a ribavirin acyclic analogue, 1-(2-hydroxyethoxymethyl)-1,2,4-triazole-3-carboxamide, has been determined by X-ray diffraction method. The space group is P1, unit cell parameters: a = 5,237, b = 6,960, c = 11,483 A, alpha = 93,89, beta = 97,43, gamma = 94,26 degrees; Z = 2. The structure was solved by the direct method and refined by least-squares procedure to R = 3.7%. Two molecular conformers statistically coexist in the unit cell, differing in the hydroxyethoxymethyl group conformation. Trans-conformation about O4'-C4' bond and gauche about C4'-C5' bond are observed in both molecules. C1'-O4' bond is approximately perpendicular to the aglicon.

[The structure and antiviral activity of ribavirin analogs. II. Molecular and crystal structure of 1-(1,5-dihydroxy-3-oxapent-2-yl)-1,2,4-triazole-5-carboxamide]. / Struktura i protivovirusnaia aktivnost' analogov ribavirina. II. Molekuliarnaia i kristallicheskaia struktura 1-(1,5-digidroksi-3-oksapent-2-il)-1,2,4-triazol-5-karboksamida.

X-ray structure of the title compound, an antiviral agent moderately active towards Herpes simplex virus type 1, has been determined. The space group is P2i/n, unit cell parameters: a = 10,119, b = 7,529, c = 13,585 A, beta = 107,82 degrees, Z = 4. The structure was solved by the direct method and refined by least-squares procedure to R = 2.9%. The gauche-conformation about C4'-C5' bond and trans-conformation about O4'-C4' bond are realized in the molecule. The carboxyamide group at the C5 atom of triazol cycle provides a steric opportunity for the intramolecular hydrogen bond C1'-H1'...O6 formation.

A new synthesis of 2'-C-methylnucleosides starting from D-ribose.

A general method have been developed for the synthesis of 2'-C-methylnucleosides from 2,3-O-isopropylidene-2-hydroxymethyl-5-O-trityl-D-ribofuranose (2).