Clusterin in the protein corona plays a key role in the stealth effect of nanoparticles against phagocytes

In biological fluids, nanoparticles interact with biological components such as proteins, and a layer called the “protein corona” forms around the nanoparticles. It is believed that the composition of the protein corona affects the cellular uptake and in vivo biodistribution of nanoparticles; howeve...

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Veröffentlicht in:Biochemical and biophysical research communications 2016-11, Vol.480 (4), p.690-695
Hauptverfasser: Aoyama, Michihiko, Hata, Katsutomo, Higashisaka, Kazuma, Nagano, Kazuya, Yoshioka, Yasuo, Tsutsumi, Yasuo
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Sprache:eng
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Zusammenfassung:In biological fluids, nanoparticles interact with biological components such as proteins, and a layer called the “protein corona” forms around the nanoparticles. It is believed that the composition of the protein corona affects the cellular uptake and in vivo biodistribution of nanoparticles; however, the key proteins of the protein corona that control the biological fate of nanoparticles remain unclear. Recently, it was reported that clusterin binding to pegylated nanoparticles is important for the stealth effect of pegylated nanoparticles in phagocytes. However, the effect of clusterin on non-pegylated nanoparticles is unknown, although it is known that clusterin is present in the protein corona of non-pegylated nanoparticles. Here, we assessed the stealth effect of clusterin in the corona of non-pegylated silver nanoparticles and silica nanoparticles. We found that serum- and plasma-protein corona inhibited the cellular uptake of silver nanoparticles and silica nanoparticles in phagocytes and that the plasma-protein corona showed a greater stealth effect compared with the serum-protein corona. Clusterin was present in both the serum- and plasma-protein corona, but was present at a higher level in the plasma-protein corona than in the serum-protein corona. Clusterin binding to silver nanoparticles and silica nanoparticles suppressed the cellular uptake of nanoparticles in human macrophage-like cells (THP-1 cells). Although further studies are required to determine how clusterin suppresses non-specific cellular uptake in phagocytes, our data suggest that clusterin plays a key role in the stealth effect of not only pegylated nanoparticles but also non-pegylated nanoparticles. •Protein corona inhibit the uptake of silver or silica nanoparticles by phagocytes.•Clusterin levels were higher in plasma-protein corona than in serum-protein corona.•Clusterin inhibited the cellular uptake of silver or silica nanoparticles.
ISSN:0006-291X
1090-2104
DOI:10.1016/j.bbrc.2016.10.121