Impact of dose and surface features on plasmatic and liver concentrations of biodegradable polymeric nanocapsules.
Data
2017
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Resumo
The effect of polymeric nanocapsule dose on plasmatic and liver concentrations 20 min after intravenous
administration in mice was evaluated. Nanocapsules were prepared with different polymers, namely, poly(D,Llactide)
(PLA), polyethylene glycol-block-poly(D,L-lactide) (PLA-PEG), and PLA with chitosan (PLA-Cs) and
compared with a nanoemulsion. These formulations were labelled with a phthalocyanine dye for fluorescent
detection. The nanostructures had narrow size distributions upon separation by asymmetric flow field flow
fractionation with static and dynamic light scattering detection, with average hydrodynamic diameters in the
130–300 nm range, negative zeta potentials, except PLA-Cs nanocapsules, which had a positive zeta potential.
Flow cytometry revealed uptake mostly by monocytes and neutrophils in mice and human blood. PLA
nanocapsules and the nanoemulsion showed dose-dependent plasma concentrations, where the percentage of
plasmatic fluorescence increased with increasing administered dose. In contrast, PLA-PEG nanocapsules led to a
dose-independent plasmatic profile. PLA-Cs nanocapsules showed the lowest plasmatic and liver levels of
fluorescence at all administered doses and significant intravenous toxicity in mice. This work demonstrates the
importance of considering the nanocarrier dose when evaluating pharmacokinetic and biodistribution data and
emphasizes the role of surface features in determining the plasmatic and liver concentrations of a poorly soluble
lipophilic encapsulated compound.
Descrição
Palavras-chave
Chitosan, Polymer dose, Phthalocyanine, Field flow fractionation
Citação
OLIVEIRA, L. T. et al. Impact of dose and surface features on plasmatic and liver concentrations of biodegradable polymeric nanocapsules. European Journal Of Pharmaceutical Sciences, v. 105, p. 19-32, 2017. Disponível em: <http://www.sciencedirect.com/science/article/pii/S0928098717302117?via%3Dihub>. Acesso em: 29 ago. 2017.