Imaging breast cancer using a dual-ligand nanochain particle.

Nanoparticles often only exploit the upregulation of a receptor on cancer cells to enhance intratumoral deposition of therapeutic and imaging agents. However, a single targeting moiety assumes that a tumor is homogenous and static. Tumoral microenvironments are both heterogenous and dynamic, often d...

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Main Authors: Gil Covarrubias, Anthony Cha, Abdelrahman Rahmy, Morgan Lorkowski, Vindya Perera, Bernadette O Erokwu, Chris Flask, Pubudu M Peiris, William P Schiemann, Efstathios Karathanasis
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2018-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC6193613?pdf=render
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spelling doaj-478e9edf1e1b4fa4a06a9a29dd55192c2020-11-25T02:33:21ZengPublic Library of Science (PLoS)PLoS ONE1932-62032018-01-011310e020429610.1371/journal.pone.0204296Imaging breast cancer using a dual-ligand nanochain particle.Gil CovarrubiasAnthony ChaAbdelrahman RahmyMorgan LorkowskiVindya PereraBernadette O ErokwuChris FlaskPubudu M PeirisWilliam P SchiemannEfstathios KarathanasisNanoparticles often only exploit the upregulation of a receptor on cancer cells to enhance intratumoral deposition of therapeutic and imaging agents. However, a single targeting moiety assumes that a tumor is homogenous and static. Tumoral microenvironments are both heterogenous and dynamic, often displaying variable spatial and temporal expression of targetable receptors throughout disease progression. Here, we evaluated the in vivo performance of an iron oxide nanoparticle in terms of targeting and imaging of orthotropic mouse models of aggressive breast tumors. The nanoparticle, a multi-component nanochain, was comprised of 3-5 iron oxide nanoparticles chemically linked in a linear chain. The nanoparticle's surface was decorated with two types of ligands each targeting two different upregulated biomarkers on the tumor endothelium, P-selectin and fibronectin. The nanochain exhibited improved tumor deposition not only through vascular targeting but also through its elongated structure. A single-ligand nanochain exhibited a ~2.5-fold higher intratumoral deposition than a spherical nanoparticle variant. Furthermore, the dual-ligand nanochain exhibited higher consistency in generating detectable MR signals compared to a single-ligand nanochain. Using a 7T MRI, the dual-ligand nanochains exhibited highly detectable MR signal within 3h after injection in two different animal models of breast cancer.http://europepmc.org/articles/PMC6193613?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Gil Covarrubias
Anthony Cha
Abdelrahman Rahmy
Morgan Lorkowski
Vindya Perera
Bernadette O Erokwu
Chris Flask
Pubudu M Peiris
William P Schiemann
Efstathios Karathanasis
spellingShingle Gil Covarrubias
Anthony Cha
Abdelrahman Rahmy
Morgan Lorkowski
Vindya Perera
Bernadette O Erokwu
Chris Flask
Pubudu M Peiris
William P Schiemann
Efstathios Karathanasis
Imaging breast cancer using a dual-ligand nanochain particle.
PLoS ONE
author_facet Gil Covarrubias
Anthony Cha
Abdelrahman Rahmy
Morgan Lorkowski
Vindya Perera
Bernadette O Erokwu
Chris Flask
Pubudu M Peiris
William P Schiemann
Efstathios Karathanasis
author_sort Gil Covarrubias
title Imaging breast cancer using a dual-ligand nanochain particle.
title_short Imaging breast cancer using a dual-ligand nanochain particle.
title_full Imaging breast cancer using a dual-ligand nanochain particle.
title_fullStr Imaging breast cancer using a dual-ligand nanochain particle.
title_full_unstemmed Imaging breast cancer using a dual-ligand nanochain particle.
title_sort imaging breast cancer using a dual-ligand nanochain particle.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2018-01-01
description Nanoparticles often only exploit the upregulation of a receptor on cancer cells to enhance intratumoral deposition of therapeutic and imaging agents. However, a single targeting moiety assumes that a tumor is homogenous and static. Tumoral microenvironments are both heterogenous and dynamic, often displaying variable spatial and temporal expression of targetable receptors throughout disease progression. Here, we evaluated the in vivo performance of an iron oxide nanoparticle in terms of targeting and imaging of orthotropic mouse models of aggressive breast tumors. The nanoparticle, a multi-component nanochain, was comprised of 3-5 iron oxide nanoparticles chemically linked in a linear chain. The nanoparticle's surface was decorated with two types of ligands each targeting two different upregulated biomarkers on the tumor endothelium, P-selectin and fibronectin. The nanochain exhibited improved tumor deposition not only through vascular targeting but also through its elongated structure. A single-ligand nanochain exhibited a ~2.5-fold higher intratumoral deposition than a spherical nanoparticle variant. Furthermore, the dual-ligand nanochain exhibited higher consistency in generating detectable MR signals compared to a single-ligand nanochain. Using a 7T MRI, the dual-ligand nanochains exhibited highly detectable MR signal within 3h after injection in two different animal models of breast cancer.
url http://europepmc.org/articles/PMC6193613?pdf=render
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