Literature DB >> 16848398

Self-assembled quantum dot-peptide bioconjugates for selective intracellular delivery.

James B Delehanty1, Igor L Medintz, Thomas Pons, Florence M Brunel, Philip E Dawson, Hedi Mattoussi.   

Abstract

We demonstrate the use of self-assembled luminescent semiconductor quantum dot (QD)-peptide bioconjugates for the selective intracellular labeling of several eukaryotic cell lines. A bifunctional oligoarginine cell penetrating peptide (based on the HIV-1 Tat protein motif) bearing a terminal polyhistidine tract was synthesized and used to facilitate the transmembrane delivery of the QD bioconjugates. The polyhistidine sequence allows the peptide to self-assemble onto the QD surface via metal-affinity interactions while the oligoarginine sequence allows specific QD delivery across the cellular membrane and intracellular labeling as compared to nonconjugated QDs. This peptide-driven delivery is concentration-dependent and thus can be titrated. Upon internalization, QDs display a punctate-like staining pattern in which some, but not all, of the QD signal is colocalized within endosomes. The effects of constant versus limited exposure to QD-peptide conjugates on cellular viability are evaluated by a metabolic specific assay, and clear differences in cytotoxicity are observed. The efficacy of using peptides for selective intracellular delivery is highlighted by performing a multicolor QD labeling, where we found that the presence or absence of peptide on the QD surface controls cellular uptake.

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Year:  2006        PMID: 16848398      PMCID: PMC2519024          DOI: 10.1021/bc060044i

Source DB:  PubMed          Journal:  Bioconjug Chem        ISSN: 1043-1802            Impact factor:   4.774


  45 in total

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6.  Cationic TAT peptide transduction domain enters cells by macropinocytosis.

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8.  Cellular uptake of unconjugated TAT peptide involves clathrin-dependent endocytosis and heparan sulfate receptors.

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9.  Cell membrane lipid rafts mediate caveolar endocytosis of HIV-1 Tat fusion proteins.

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  48 in total

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4.  Study on the intracellular fate of Tat peptide-conjugated quantum dots by spectroscopic investigation.

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6.  Influence of the metal center and linker on the intracellular distribution and biological activity of organometal-peptide conjugates.

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7.  Quantum Dot-Peptide-Fullerene Bioconjugates for Visualization of in Vitro and in Vivo Cellular Membrane Potential.

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8.  Quantum dot-mediated delivery of siRNA to inhibit sphingomyelinase activities in brain-derived cells.

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9.  Selecting improved peptidyl motifs for cytosolic delivery of disparate protein and nanoparticle materials.

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Review 10.  State of academic knowledge on toxicity and biological fate of quantum dots.

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