The PEG-Fluorochrome Shielding Approach for Targeted Probe Design

We provide a new approach for fluorescent probe design termed “PEG-fluorochrome shielding”, where PEGylation enhances quantum yields while blocking troublesome interactions between fluorochromes and biomolecules. To demonstrate PEG-fluorochrome shielding, fluorochrome-bearing peptide probes were syn...

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Published inJournal of the American Chemical Society Vol. 134; no. 47; pp. 19338 - 19341
Main Authors Guo, Yanyan, Yuan, Hushan, Rice, William L, Kumar, Anand T. N, Goergen, Craig J, Jokivarsi, Kimmo, Josephson, Lee
Format Journal Article
LanguageEnglish
Published WASHINGTON American Chemical Society 28.11.2012
Amer Chemical Soc
Subjects
absorption
Animals
Cell Line, Tumor
chemical bonding
Chemistry
Chemistry, Multidisciplinary
fluorescence
fluorescent dyes
Fluorescent Dyes - administration & dosage
Fluorescent Dyes - chemistry
Humans
integrins
Mice
Molecular Probes - administration & dosage
Molecular Probes - chemical synthesis
Molecular Structure
Peptides - administration & dosage
Peptides - chemical synthesis
Physical Sciences
Polyethylene Glycols - administration & dosage
Polyethylene Glycols - chemistry
Science & Technology
NANOPARTICLE
CANCER
DYES
Online AccessGet full text
ISSN0002-7863
1520-5126
1520-5126
DOI10.1021/ja309085b

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Summary:We provide a new approach for fluorescent probe design termed “PEG-fluorochrome shielding”, where PEGylation enhances quantum yields while blocking troublesome interactions between fluorochromes and biomolecules. To demonstrate PEG-fluorochrome shielding, fluorochrome-bearing peptide probes were synthesized, three without PEG and three with a 5 kDa PEG functional group. In vitro, PEG blocked the interactions of fluorochrome-labeled peptide probes with each other (absorption spectra, self-quenching) and reduced nonspecific interactions with cells (by FACS). In vivo, PEG blocked interactions with biomolecules that lead to probe retention (by surface fluorescence). Integrin targeting in vivo was obtained as the differential uptake of an 111In-labeled, fluorochrome-shielded, integrin-binding RGD probe and a control RAD. Using PEG to block fluorochrome-mediated interactions, rather than synthesizing de novo fluorochromes, can yield new approaches for the design of actively or passively targeted near-infrared fluorescent probes.
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ISSN:0002-7863
1520-5126
1520-5126
DOI:10.1021/ja309085b