Peptide-Conjugated Ultrasmall Gold Nanoparticles (2 nm) for Selective Protein Targeting

Peptide-Conjugated Ultrasmall Gold Nanoparticles (2 nm) for Selective Protein Targeting

Ultrasmall gold nanoparticles with a metallic core diameter of 2 nm were surface-conjugated with peptides that selectively target epitopes on the surface of the WW domain of the model protein hPin1 (hPin1-WW). The binding to the gold surface was accomplished via the thiol group of a terminal cystein...

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Veröffentlicht in:ACS applied bio materials 2021-01, Vol.4 (1), p.945-965
Hauptverfasser: Ruks, Tatjana, Loza, Kateryna, Heggen, Marc, Prymak, Oleg, Sehnem, Andre Luiz, Oliveira, Cristiano L. P, Bayer, Peter, Beuck, Christine, Epple, Matthias
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container_issue 1
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container_title ACS applied bio materials
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creator Ruks, Tatjana
Loza, Kateryna
Heggen, Marc
Prymak, Oleg
Sehnem, Andre Luiz
Oliveira, Cristiano L. P
Bayer, Peter
Beuck, Christine
Epple, Matthias
description Ultrasmall gold nanoparticles with a metallic core diameter of 2 nm were surface-conjugated with peptides that selectively target epitopes on the surface of the WW domain of the model protein hPin1 (hPin1-WW). The binding to the gold surface was accomplished via the thiol group of a terminal cysteine. The particles were analyzed by NMR spectroscopy, high-resolution transmission electron microscopy, and differential centrifugal sedimentation. The surface loading was determined by conjugating a FAM-labeled peptide, followed by UV–vis spectroscopy, and by quantitative 1H NMR spectroscopy, showing about 150 peptide molecules conjugated to each nanoparticle. The interaction between the peptide-decorated nanoparticles with hPin1-WW was probed by 1H–15N-HSQC NMR titration, fluorescence polarization spectroscopy (FP), and isothermal titration calorimetry (ITC). The particles showed a similar binding (K D = 10–20 μM) compared to the dissolved peptides (K D = 10–30 μM). Small-angle X-ray scattering (SAXS) showed that the particles were well dispersed and did not agglomerate after the addition of hPin1-WW (no cross-linking by the protein). Each nanoparticle was able to bind about 20 hPin1-WW protein molecules. An unspecific interaction with hPin1 was excluded by the attachment of a nonbinding peptide to the nanoparticle surface. The uptake by cells was studied by confocal laser scanning microscopy. The peptide-functionalized nanoparticles penetrated the cell membrane and were located in the cytosol. In contrast, the dissolved peptide did not cross the cell membrane. Peptide-functionalized nanoparticles are promising agents to target proteins inside cells.
doi_str_mv 10.1021/acsabm.0c01424
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The interaction between the peptide-decorated nanoparticles with hPin1-WW was probed by 1H–15N-HSQC NMR titration, fluorescence polarization spectroscopy (FP), and isothermal titration calorimetry (ITC). The particles showed a similar binding (K D = 10–20 μM) compared to the dissolved peptides (K D = 10–30 μM). Small-angle X-ray scattering (SAXS) showed that the particles were well dispersed and did not agglomerate after the addition of hPin1-WW (no cross-linking by the protein). Each nanoparticle was able to bind about 20 hPin1-WW protein molecules. An unspecific interaction with hPin1 was excluded by the attachment of a nonbinding peptide to the nanoparticle surface. The uptake by cells was studied by confocal laser scanning microscopy. The peptide-functionalized nanoparticles penetrated the cell membrane and were located in the cytosol. In contrast, the dissolved peptide did not cross the cell membrane. 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