TY - JOUR
T1 - Receptor-mediated transcytosis
T2 - A mechanism for active extravascular transport of nanoparticles in solid tumors
AU - Lu, Wei
AU - Xiong, Chiyi
AU - Zhang, Rui
AU - Shi, Lifang
AU - Huang, Miao
AU - Zhang, Guodong
AU - Song, Shaoli
AU - Huang, Qian
AU - Liu, Gang Yu
AU - Li, Chun
N1 - Funding Information:
We thank Stephanie Deming for editing the article. This work was supported in part by grants from the National Institutes of Health (grants R01 CA119387-05S1 and RC2 GM092599 ), by the John S. Dunn Foundation , and W. M. Keck Foundation . The Transmission Electron Microscopy facility is supported by the National Institutes of Health through MD Anderson's Cancer Center Support Grant , CA016672 . The 64 Cu was provided by Washington University Medical School, which is partially funded through National Cancer Institute grant R24 CA86307 .
PY - 2012/8/10
Y1 - 2012/8/10
N2 - Targeted nanoparticle-based delivery systems have been used extensively to develop effective cancer theranostics. However, how targeting ligands affect extravascular transport of nanoparticles in solid tumors remains unclear. Here, we show, using B16/F10 melanoma cells expressing melanocortin type-1 receptor (MC1R), that the nature of targeting ligands, i.e., whether they are agonists or antagonists, directs tumor uptake and intratumoral distribution after extravasation of nanoparticles from tumor vessels into the extravascular fluid space. Pegylated hollow gold nanospheres (HAuNS, diameter = 40 nm) coated with MC1R agonist are internalized upon ligand-receptor binding, whereas MC1R antagonist-conjugated HAuNS remain attached on the cell surface. Transcellular transport of agonist-conjugated HAuNS was confirmed by a multilayer tumor cell model and by transmission electron microscopy. MC1R agonist- but not MC1R antagonist-conjugated nanoparticles exhibit significantly higher tumor uptake than nontargeted HAuNS and are quickly dispersed from tumor vessels via receptor-mediated endocytosis and subsequent transcytosis. These results confirm an active transport mechanism that can be used to overcome one of the major biological barriers for efficient nanoparticle delivery to solid tumors.
AB - Targeted nanoparticle-based delivery systems have been used extensively to develop effective cancer theranostics. However, how targeting ligands affect extravascular transport of nanoparticles in solid tumors remains unclear. Here, we show, using B16/F10 melanoma cells expressing melanocortin type-1 receptor (MC1R), that the nature of targeting ligands, i.e., whether they are agonists or antagonists, directs tumor uptake and intratumoral distribution after extravasation of nanoparticles from tumor vessels into the extravascular fluid space. Pegylated hollow gold nanospheres (HAuNS, diameter = 40 nm) coated with MC1R agonist are internalized upon ligand-receptor binding, whereas MC1R antagonist-conjugated HAuNS remain attached on the cell surface. Transcellular transport of agonist-conjugated HAuNS was confirmed by a multilayer tumor cell model and by transmission electron microscopy. MC1R agonist- but not MC1R antagonist-conjugated nanoparticles exhibit significantly higher tumor uptake than nontargeted HAuNS and are quickly dispersed from tumor vessels via receptor-mediated endocytosis and subsequent transcytosis. These results confirm an active transport mechanism that can be used to overcome one of the major biological barriers for efficient nanoparticle delivery to solid tumors.
KW - Agonists
KW - Antagonists
KW - Melanocortin type-1 receptor (MC1R)
KW - Nanoparticles
KW - Transcytosis
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U2 - 10.1016/j.jconrel.2012.05.014
DO - 10.1016/j.jconrel.2012.05.014
M3 - Article
C2 - 22617522
AN - SCOPUS:84864605778
SN - 0168-3659
VL - 161
SP - 959
EP - 966
JO - Journal of Controlled Release
JF - Journal of Controlled Release
IS - 3
ER -