Size and surface charge of gold nanoparticles determine absorption across intestinal barriers and accumulation in secondary target organs after oral administration

Schleh, Carsten; Semmler‐Behnke, Manuela; Lipka, Jens; Wenk, Alexander; Hirn, Stephanie; Schäffler, Martin; Schmid, Günter; Simon, Ulrich; Kreyling, Wolfgang G.

doi:10.3109/17435390.2011.552811

Cited by 311 publications

(248 citation statements)

References 49 publications

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“…injection in rat [6,7] and mouse [8][9][10]. The bioavailability of orally administered AuNPs has also been studied in these animal models [10][11][12]. These studies have shown that size is one of the major determinants of biodistribution [7,9,13].…”

Section: Introductionmentioning

confidence: 99%

Effect of surface coating on the biodistribution profile of gold nanoparticles in the rat

Morais

Soares

Duarte

et al. 2012

European Journal of Pharmaceutics and Biopharmaceutics

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a b s t r a c tSuccessful application of gold nanoparticles (AuNPs) in biomedicine requires extensive safety assessment for which biokinetic studies are crucial.We evaluated the biodistribution of AuNPs ($20 nm) with different surface coatings: citrate, 11-MUA and 3 pentapeptides, CALNN, CALND and CALNS, after i.v. administration to rats (0.6-1 mg Au/kg). Biodistribution was evaluated based on Au tissue content measured by GFAAS.Citrate-AuNPs were rapidly removed from circulation with 60% of the injected dose depositing in the liver. Thirty minutes post-injection, the lungs presented about 6% of the injected dose with levels decreasing to 0.7% at 24 h. Gold levels in the spleen were of 2.6%. After 24 h, liver presented the highest Au level, followed by spleen and blood.A similar biodistribution profile was observed for MUA-coated AuNPs compared to Cit-AuNPs at 24 h post-injection, while significantly higher levels of peptide-capped AuNPs were found in the liver (74-86%) accompanied by a corresponding decrease in blood levels.TEM analysis of liver slices showed AuNPs in Kupffer cells and hepatocytes, trapped inside endosomes. Our data demonstrate that AuNPs are rapidly distributed and that the liver is the preferential accumulation organ. Peptide capping significantly increased hepatic uptake, showing the influence of AuNPs functionalization in biodistribution.

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Section: Introductionmentioning

confidence: 99%

Effect of surface coating on the biodistribution profile of gold nanoparticles in the rat

Morais

Soares

Duarte

et al. 2012

European Journal of Pharmaceutics and Biopharmaceutics

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“…Biomolecules that are not replaced would serve as a corona 'memory' of the nanoparticle's previous environment. Therefore the corona composition could potentially depend not only on the current environment of the nanoparticle, but on all environments it has moved through 26,27 . Figure 2 illustrates this concept for inhaled nanoparticles carrying typical lung surfactant proteins, and other membrane components, when they reach the blood circulation 28,29 .…”

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confidence: 99%

Biomolecular coronas provide the biological identity of nanosized materials

Åberg²,

et al. 2012

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“…Therefore, it is important to elucidate the uptake pattern of the polyester NPs, particularly in hepatic cell lines, as it is well established that the liver is a site of accumulation for many nanoparticles following exposure via various routes (e.g. intravenous injection, ingestion, inhalation/intratracheal instillation) [34,35,37]. The uptake of coated and uncoated P02 NPs in C3A cells suggested that the NPs were taken up by the cells in a time and concentration dependent manner.…”

Section: Discussionmentioning

confidence: 99%

“…Hepatocytes were selected as the liver is the primary site of nanoparticle accumulation following exposure via different routes (e.g. intratracheal instillation, ingestion, intravenous injection), and existing evidence suggests that C3A cells respond similarly to primary human hepatocytes [34][35][36][37]. The internalization of coated and uncoated polymer nanoparticles by hepatocytes was assessed over time, and their effects on cell viability evaluated using three assays; Alamar Blue, Neutral Red, and 5-CFDA-AM [5-carboxyfluorescein diacetate, acetoxymethyl ester] CFDA-AM.…”

Section: Introductionmentioning

confidence: 99%

Synthesis, characterization and evaluation of in vitro toxicity in hepatocytes of linear polyesters with varied aromatic and aliphatic co-monomers

Kakde

Powell

Bansal

et al. 2016

Journal of Controlled Release

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Size and surface charge of gold nanoparticles determine absorption across intestinal barriers and accumulation in secondary target organs after oral administration

Cited by 311 publications

References 49 publications

Effect of surface coating on the biodistribution profile of gold nanoparticles in the rat

Effect of surface coating on the biodistribution profile of gold nanoparticles in the rat

Biomolecular coronas provide the biological identity of nanosized materials

Synthesis, characterization and evaluation of in vitro toxicity in hepatocytes of linear polyesters with varied aromatic and aliphatic co-monomers

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