4.8 Article

Improved stability and biocompatibility of nanostructured silicon drug carrier for intravenous administration

Journal

ACTA BIOMATERIALIA
Volume 13, Issue -, Pages 207-215

Publisher

ELSEVIER SCI LTD
DOI: 10.1016/j.actbio.2014.11.019

Keywords

Porous silicon nanoparticles; Polyethylene glycol; Surface modification; Biocompatilibity; Opsonization

Funding

  1. University of Eastern Finland (NAMBER consortium)
  2. University of Helsinki
  3. Academy of Finland [252215, 256394]
  4. Biocentrum Helsinki
  5. European Research Council under the European Union [310892]
  6. Academy of Finland (AKA) [256394, 256394] Funding Source: Academy of Finland (AKA)
  7. European Research Council (ERC) [310892] Funding Source: European Research Council (ERC)

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Nanotechnology has attracted considerable interest in the field of biomedicine, where various nanopartides (NPs) have been introduced as efficient drug carrier systems. Mesoporous silicon (PSi) is one of the most promising materials in this field due to its low toxicity, good biodegradability, high surface area, tunable pore size and controllable surface functionality. However, recognition by the reticuloendothelial system and particle agglomeration hinder the use of PSi for intravenous applications. The present paper describes a dual-PEGylation method, where two PEG molecules with different sizes (0.5 and 2 kDa) were grafted simultaneously in a single process onto thermally oxidized PSi NPs to form a high-density PEG coating with both brush-like and mushroom-like conformation. The material was characterized in detail and the effects of the dual-PEGylation on cell viability, protein adsorption and macrophage uptakes were evaluated. The results show that dual-PEGylation improves the colloidal stability of the NPs in salt solutions, prolongs their half-lives, and minimizes both protein adsorption and macrophage uptake. Therefore, these new dual-PEGylated PSi NPs are potential candidates for intravenous applications. (C) 2014 Acta Materialia Inc. Published by Elsevier Ltd. All rights reserved.

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