Nanoparticle-based drug delivery via RBC-hitchhiking for the inhibition of lung metastases growth

Delivery of particle-based theranostic agents via their transportation on the surfaces of red blood cells, commonly referred to as RBC-hitchhiking, has historically been developed as a promising strategy for increasing the extremely poor blood circulation lifetime, primarily, of the large-sized sub-...

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Veröffentlicht in:	Nanoscale 2019-01, Vol.11 (4), p.1636-1646
Hauptverfasser:	Zelepukin, I V, Yaremenko, A V, Shipunova, V O, Babenyshev, A V, Balalaeva, I V, Nikitin, P I, Deyev, S M, Nikitin, M P
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Sprache:	eng
Schlagworte:	Blood circulation Cancer Drug delivery systems Erythrocytes Lungs Metastasis Nanoparticles Polymer coatings Prolongation
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creator	Zelepukin, I V Yaremenko, A V Shipunova, V O Babenyshev, A V Balalaeva, I V Nikitin, P I Deyev, S M Nikitin, M P
description	Delivery of particle-based theranostic agents via their transportation on the surfaces of red blood cells, commonly referred to as RBC-hitchhiking, has historically been developed as a promising strategy for increasing the extremely poor blood circulation lifetime, primarily, of the large-sized sub-micron agents. Here, we show for the first time that RBC-hitchhiking can be extremely efficient for nanoparticle delivery and tumor treatment even in those cases when no circulation prolongation is observed. Specifically, we demonstrate that RBC-hitchhiking of certain small 100 nm particles, unlike that of the conventional sub-micron ones, can boost the delivery of non-targeted particles to lungs up to a record high value of 120-fold (and up to 40% of the injected dose). To achieve this remarkable result, we screened sub-200 nm nanoparticles of different sizes, polymer coatings and ζ-potentials and identified particles with the optimal RBC adsorption/desorption behavior. Furthermore, we demonstrated that such RBC-mediated rerouting of particles to lungs can be used to fight pulmonary metastases of aggressive melanoma B16-F1. Our findings could change the general paradigm of drug delivery for cancer treatment with RBC-hitchhiking. It is not the blood circulation lifetime that is the key factor for nanoparticle efficiency, but rather the complexation of nanoparticles with the RBC. The demonstrated technology could become a valuable tool for development of new strategies based on small nanoparticles for the treatment of aggressive and small-cell types of cancer as well as other lung diseases.
doi_str_mv	10.1039/c8nr07730d
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Here, we show for the first time that RBC-hitchhiking can be extremely efficient for nanoparticle delivery and tumor treatment even in those cases when no circulation prolongation is observed. Specifically, we demonstrate that RBC-hitchhiking of certain small 100 nm particles, unlike that of the conventional sub-micron ones, can boost the delivery of non-targeted particles to lungs up to a record high value of 120-fold (and up to 40% of the injected dose). To achieve this remarkable result, we screened sub-200 nm nanoparticles of different sizes, polymer coatings and ζ-potentials and identified particles with the optimal RBC adsorption/desorption behavior. Furthermore, we demonstrated that such RBC-mediated rerouting of particles to lungs can be used to fight pulmonary metastases of aggressive melanoma B16-F1. Our findings could change the general paradigm of drug delivery for cancer treatment with RBC-hitchhiking. 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source	Royal Society Of Chemistry Journals 2008-
subjects	Blood circulation Cancer Drug delivery systems Erythrocytes Lungs Metastasis Nanoparticles Polymer coatings Prolongation
title	Nanoparticle-based drug delivery via RBC-hitchhiking for the inhibition of lung metastases growth
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