Publication Type Journal Article
Title Interrogating the Role of Receptor-Mediated Mechanisms: Biological Fate of Peptide-Functionalized Radiolabeled Gold Nanoparticles in Tumor Mice
Authors Francisco Silva Ajit Zambre Maria Paula C. Campello Lurdes Gano Isabel Santos Ana Maria Ferraria M J Ferreira Amolak Singh Anandhi Upendran Antonio Paulo Raghuraman Kannan
Groups BioMol
Journal BIOCONJUGATE CHEMISTRY
Year 2016
Month April
Volume 27
Number 4
Pages 1153-1164
Abstract To get a better insight on the transport mechanism of peptide-conjugated nanoparticles to tumors, we performed in vivo biological studies of bombesin (BBN) peptide functionalized gold nanoparticles (AuNPs) in human prostate tumor bearing mice. Initially, we sought to compare AuNPs with thiol derivatives of acyclic and macrocyclic chelators of DTPA and DOTA types. The DTPA derivatives were unable to provide a stable coordination of Ga-67, and therefore, the functionalization with the BBN analogues was pursued for the DOTA-containing AuNPs. The DOTA-coated AuNPs were functionalized with BBN[7-14] using a unidentate cysteine group or a bidentate thioctic group to attach the peptide. AuNPs functionalized with thioctic-BBN displayed the highest in vitro cellular internalization (approximate to 25\%, 15 min) in gastrin releasing peptide (GRP) receptor expressing cancer cells. However, these results fail to translate to in vivo tumor uptake. Biodistribution studies following intravenous (IV) and intraperitoneal (IP) administration of nanoconjugates in tumor bearing mice indicated that the presence of BBN influences to some degree the biological profile of the nanoconstructs. For IV administration, the receptor-mediated pathway appears to be outweighed by the EPR effect. By contrast, in IP administration, it is reasoned that the GRPr-mediated mechanism plays a role in pancreas uptake.
DOI http://dx.doi.org/10.1021/acs.bioconjchem.6b00102
ISBN
Publisher AMER CHEMICAL SOC
Book Title
ISSN 1043-1802
EISSN
Conference Name
Bibtex ID ISI:000374812600033
Observations
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