4.8 Article

Targeting Nanoparticles to Bioengineered Human Vascular Networks

Journal

NANO LETTERS
Volume 21, Issue 15, Pages 6609-6616

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acs.nanolett.1c02027

Keywords

phototargeted nanoparticle; micelle; bioengineered human vascular network; tissue engineering; vascular anomalies

Funding

  1. NIH [R35 GM131728]
  2. Stuart and Jane Weitzman Family Vascular Anomalies Fund

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Targeted nanoparticle drug delivery systems have the potential to enhance drug accumulation within bioengineered human vascular networks, demonstrating significantly increased drug levels compared to off-target sites without targeting. This approach has the potential to greatly improve drug delivery to vascular anomalies.
Pharmacotherapy of vascular anomalies has limited efficacy and potentially limiting toxicity. Targeted nanoparticle (NP) drug delivery systems have the potential to accumulate within tissues where the vasculature is impaired, potentially leading to high drug levels (increased efficacy) in the diseased tissue and less in off-target sites (less toxicity). Here, we investigate whether NPs can be used to enhance drug delivery to bioengineered human vascular networks (hVNs) that are a model of human vascular anomalies. We demonstrate that intravenously injected phototargeted NPs enhanced accumulation of NPs and the drug within hVNs. With phototargeting we demonstrate 17 times more NP accumulation within hVNs than was detected in hVNs without phototargeting. With phototargeting there was 10-fold more NP accumulation within hVNs than in any other organ. Phototargeting resulted in a 6-fold increase in drug accumulation (doxorubicin) within hVNs in comparison to animals injected with the free drug. Nanoparticulate approaches have the potential to markedly improve drug delivery to vascular anomalies.

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