4.5 Article

Biodistribution of Fluorescent Albumin Nanoparticles among Organs of Laboratory Animals after Intranasal and Peroral Administration

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CURRENT ISSUES IN MOLECULAR BIOLOGY
卷 45, 期 10, 页码 8227-8238

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MDPI
DOI: 10.3390/cimb45100519

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fluorescent BSA nanoparticles; nanoprecipitation; stability in blood sera and saliva; intranasal and peroral administration; dynamics of biodistribution in organs of mice; penetration in brain and intestine; absence of interferon gene expression induction

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This study investigated the stability and distribution of protein nanoparticles (NP) in biological fluids and organs after intranasal and oral administration. The results showed that the labeled BSA NP remained stable in blood sera and nasopharyngeal swabs and mainly accumulated in the brain and intestine without inducing innate immunity.
Natural, environmental and engineered nanoparticles (NP) penetrate into cells by endocytosis and induce innate immunity. The behaviour of the nanomaterials both in vitro and in vivo should be assessed. Our goal was to study protein NP stability in biological fluids and distribution in organs of animals after intranasal and oral administration. Bovine serum albumin (BSA) was labelled with the fluorescent dye RhoB and NP were fabricated by nanoprecipitation. The fluorescent protein NPwere administered intranasally and orally in laboratory-outbred mice ICR and rabbits. RhoB-BSA NP distribution in organs was detected using spectrofluorometry and fluorescent microscopy. Innate immunity was evaluated using reverse transcription with random hexanucleotide primer and subsequent real-time PCR with specific fluorescent hydrolysis probes. The labelled BSA NP were shown to remain stable in blood sera and nasopharyngeal swabs for 5 days at +37 degrees C. In vivo the maximal accumulation was found in the brain in 2 days posttreatment without prevalent accumulation in olfactory bulbs. For the intestine, heart and liver, the BSA NP accumulation was similar in 1 and 2 days, whereas for kidney samples even decreased after 1 day. Both intranasal and peroral administration of RhoB-BSA NP did not induce innate immunity. Thus, after intranasal or oral instillation RhoB-BSA NP were found mainly in the brain and intestine without interferon gene expression.

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