On the formation of protein corona on colloidal nanoparticles stabilized by depletant polymers

On the formation of protein corona on colloidal nanoparticles stabilized by depletant polymers

To counter the undesired colloidal destabilization of nanoparticles in biologically-compatible media of high ionic strength (i.e. NaCl, phosphate buffer), polymers can be added to nanoparticle suspensions that will be used in biomedical applications. In these suspensions, polymers can promote high c...

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Veröffentlicht in:Materials Science & Engineering C 2019-12, Vol.105, p.110080-110080, Article 110080
Hauptverfasser: Petry, Romana, Saboia, Viviane M., Franqui, Lidiane S., Holanda, Camila de A., Garcia, Thiago R.R., de Farias, Marcelo A., de Souza Filho, Antonio G., Ferreira, Odair P., Martinez, Diego S.T., Paula, Amauri J.
Format: Artikel
Sprache:eng
Schlagworte:
Addition polymerization
Animals
Biocompatibility
Biomedical materials
Biomolecules
Blood plasma
Bovine serum albumin
Buffers
Cattle
Colloids
Depletion
Destabilization
Human blood plasma
Humans
Ionic strength
Materials science
Nanoparticles
Nanoparticles - chemistry
Phosphates
Pluronic F-127
Poloxamer - chemistry
Poly(ethylene glycol)
Polyethylene glycol
Polyethylene Glycols - chemistry
Polymers
Protein composition
Protein corona
Protein Corona - chemistry
Proteins
Repulsive depletion forces
Serum albumin
Serum Albumin, Bovine - chemistry
Silica
Silicon dioxide
Silicon Dioxide - chemistry
Sodium chloride
Stability
Stabilizers (agents)
Stöber silica nanoparticles
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Zusammenfassung:To counter the undesired colloidal destabilization of nanoparticles in biologically-compatible media of high ionic strength (i.e. NaCl, phosphate buffer), polymers can be added to nanoparticle suspensions that will be used in biomedical applications. In these suspensions, polymers can promote high colloidal stability by manifestation of steric and/or depletion forces. However, little is known about the influence of these polymers on the interactions between nanoparticles and the biological components of the organism, such as proteins and cells. In this work, it was shown that the addition of the polymers (i) Pluronic-F127 (PF127), (ii) polyethylene glycol (PEG) of different molecular weights – 1.5, 12 and 35 kDa – and (iii) the protein bovine serum albumin (BSA) on colloidal silica nanoparticles (CSNPs; 135 nm) dispersed in phosphate-buffered saline (PBS) largely alter their colloidal stability through different mechanisms. Although all polymers were adsorbed on the CSNP surface, BSA maintained the CSNP dispersion in the medium by electrosteric stabilization mechanisms, while PEG and PF127 led to the occurrence of depletion forces between the particles. In addition, it was found that the interactions between polymers and CSNPs did not prevent proteins to access the nanoparticles' surface and have minimal effect on the formation of the protein corona when they were incubated in human blood plasma. On the other hand, BSA had a greater effect on the CSNP protein corona profile compared to other polymers (PEG and PF127). Together, these results confirm that biocompatible polymers PEG and PF127 can be used as colloidal stabilizing agents for nanoparticles since they preserve the accessibility of biomolecules to the nanoparticle surface, and they have little effect on the protein corona composition. [Display omitted] •PEG and PF127 create depletion forces in colloids of silica nanoparticles (SCNPs) dispersed in media of high ionic strength.•Depletion forces manifested by PF127 can promote colloidal stabilization of nanoparticles in physiological medium (PBS).•Although PEG and PF127 adsorb on the SCNPs surfaces, plasma proteins replace these polymers in a later adsorption.•SCNPs suspension stabilized with PEG and PF127 by depletion forces did not have the protein corona composition altered.
ISSN:0928-4931
1873-0191
DOI:10.1016/j.msec.2019.110080