Literature DB >> 28065731

Mechanisms that determine nanocarrier targeting to healthy versus inflamed lung regions.

Jacob S Brenner1, Kartik Bhamidipati2, Patrick M Glassman2, N Ramakrishnan3, Depeng Jiang4, Andrew J Paris5, Jacob W Myerson2, Daniel C Pan2, Vladimir V Shuvaev2, Carlos H Villa2, Elizabeth D Hood2, Raisa Kiseleva2, Colin F Greineder2, Ravi Radhakrishnan3, Vladimir R Muzykantov6.   

Abstract

Inflamed organs display marked spatial heterogeneity of inflammation, with patches of inflamed tissue adjacent to healthy tissue. To investigate how nanocarriers (NCs) distribute between such patches, we created a mouse model that recapitulates the spatial heterogeneity of the inflammatory lung disease ARDS. NCs targeting the epitope PECAM strongly accumulated in the lungs, but were shunted away from inflamed lung regions due to hypoxic vasoconstriction (HVC). In contrast, ICAM-targeted NCs, which had lower whole-lung uptake than PECAM/NCs in inflamed lungs, displayed markedly higher NC levels in inflamed regions than PECAM/NCs, due to increased regional ICAM. Regional HVC, epitope expression, and capillary leak were sufficient to predict intra-organ of distribution of NCs, antibodies, and drugs. Importantly, these effects were not observable with traditional spatially-uniform models of ARDS, nor when examining only whole-organ uptake. This study underscores how examining NCs' intra-organ distribution in spatially heterogeneous animal models can guide rational NC design.
Copyright © 2017 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  ARDS; Inflammation; Nano-bio interface; Nanocarriers; Nanoparticle biological interactions; Nanoparticles; Patchy; Spatial heterogeneity; Whole organ distribution

Mesh:

Substances:

Year:  2017        PMID: 28065731      PMCID: PMC5518469          DOI: 10.1016/j.nano.2016.12.019

Source DB:  PubMed          Journal:  Nanomedicine        ISSN: 1549-9634            Impact factor:   5.307


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