Literature DB >> 20498042

G protein-coupled receptors function as logic gates for nanoparticle binding and cell uptake.

Wolfgang Hild1, Klaus Pollinger, Andrea Caporale, Chiara Cabrele, Max Keller, Nicola Pluym, Armin Buschauer, Reinhard Rachel, Joerg Tessmar, Miriam Breunig, Achim Goepferich.   

Abstract

More selective interactions of nanoparticles with cells would substantially increase their potential for diagnostic and therapeutic applications. Thus, it would not only be highly desirable that nanoparticles can be addressed to any cell with high target specificity and affinity, but that we could unequivocally define whether they rest immobilized on the cell surface as a diagnostic tag, or if they are internalized to serve as a delivery vehicle for drugs. To date no class of targets is known that would allow direction of nanoparticle interactions with cells alternatively into one of these mutually exclusive events. Using MCF-7 breast cancer cells expressing the human Y(1)-receptor, we demonstrate that G protein-coupled receptors provide us with this option. We show that quantum dots carrying a surface-immobilized antagonist remain with nanomolar affinity on the cell surface, and particles carrying an agonist are internalized upon receptor binding. The receptor functions like a logic "and-gate" that grants cell access only to those particles that carry a receptor ligand "and" where the ligand is an agonist. We found that agonist- and antagonist-modified nanoparticles bind to several receptor molecules at a time. This multiligand binding leads to five orders of magnitude increased-receptor affinities, compared with free ligand, in displacement studies. More than 800 G protein-coupled receptors in humans provide us with the paramount advantage that targeting of a plethora of cells is possible, and that switching from cell recognition to cell uptake is simply a matter of nanoparticle surface modification with the appropriate choice of ligand type.

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Year:  2010        PMID: 20498042      PMCID: PMC2890824          DOI: 10.1073/pnas.0912782107

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  33 in total

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Journal:  Biomaterials       Date:  2005-04-15       Impact factor: 12.479

8.  Neuropeptide Y: complete amino acid sequence of the brain peptide.

Authors:  K Tatemoto
Journal:  Proc Natl Acad Sci U S A       Date:  1982-09       Impact factor: 11.205

9.  Gastrin releasing protein receptor specific gold nanorods: breast and prostate tumor avid nanovectors for molecular imaging.

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Review 10.  The biology of VEGF and its receptors.

Authors:  Napoleone Ferrara; Hans-Peter Gerber; Jennifer LeCouter
Journal:  Nat Med       Date:  2003-06       Impact factor: 53.440

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  18 in total

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Review 2.  Quantum dots in cell biology.

Authors:  Margarida M Barroso
Journal:  J Histochem Cytochem       Date:  2011-03       Impact factor: 2.479

Review 3.  Applications of nanotechnology in dermatology.

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Journal:  J Invest Dermatol       Date:  2012-01-05       Impact factor: 8.551

Review 4.  Targeting receptor-mediated endocytotic pathways with nanoparticles: rationale and advances.

Authors:  Shi Xu; Bogdan Z Olenyuk; Curtis T Okamoto; Sarah F Hamm-Alvarez
Journal:  Adv Drug Deliv Rev       Date:  2012-09-29       Impact factor: 15.470

5.  Influenza A virus mimetic nanoparticles trigger selective cell uptake.

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6.  A Systematic Evaluation of Factors Affecting Extracellular Vesicle Uptake by Breast Cancer Cells.

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Journal:  Tissue Eng Part A       Date:  2017-07-20       Impact factor: 3.845

Review 7.  Application of advances in endocytosis and membrane trafficking to drug delivery.

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Journal:  Adv Drug Deliv Rev       Date:  2020-08-03       Impact factor: 15.470

Review 8.  Interactions of nanomaterials and biological systems: Implications to personalized nanomedicine.

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Journal:  Adv Drug Deliv Rev       Date:  2012-08-17       Impact factor: 15.470

9.  Maltoheptaose promotes nanoparticle internalization by Escherichia coli.

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10.  Silver nanoparticles (Ag-NPs) in the central amygdala protect the rat conditioned by morphine from withdrawal attack due to naloxone via high-level nitric oxide.

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