Use of a polycation spacer for noncovalent immobilization of albumin on thermally modified virus particles

The noncovalent immobilization of the protein bovine serum albumin on the surface of spherical nanoparticles 330 ± 60 nm in diameter is described. These nanoparticles are prepared by the thermal treatment of tobacco mosaic virus and are preliminarily covered with a layer of the cationic polymer poly...

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Veröffentlicht in:Polymer science. Series A, Chemistry, physics Chemistry, physics, 2011-11, Vol.53 (11), p.1026-1031
Hauptverfasser: Nikitin, N. A., Malinin, A. S., Rakhnyanskaya, A. A., Trifonova, E. A., Karpova, O. V., Yaroslavov, A. A., Atabekov, J. G.
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Sprache:eng
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Zusammenfassung:The noncovalent immobilization of the protein bovine serum albumin on the surface of spherical nanoparticles 330 ± 60 nm in diameter is described. These nanoparticles are prepared by the thermal treatment of tobacco mosaic virus and are preliminarily covered with a layer of the cationic polymer poly( N -ethyl-4-vinylpyridinium bromide). The electrostatic adsorption of the polycation on the surface of negatively charged spherical nanoparticles (on average 1.2 × 10 4 macromolecules per particle) is accompanied by recharging of the surface; as a result, the negatively charged protein bovine serum albumin can be adsorbed on it in an amount of 1.7 × 10 4 molecules per particle. The modification of spherical nanoparticles with the polycation and protein does not cause the aggregation of particles. The spherical-nanoparticle-polycation-protein ternary complex demonstrates increased stability in salt solutions relative to the spherical-nanoparticle-polycation binary complex. Because of the simplicity of the method used to modify the surface of spherical nanoparticles, it shows promise for preparation of functionally active complexes.
ISSN:0965-545X
1555-6107
DOI:10.1134/S0965545X11110083