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The Role of Negative Charge in the Delivery of Quantum Dots to Neurons

Despite our extensive knowledge of the structure of negatively charged cell surface proteoglycans and sialoglycoconjugates in the brain, we have little understanding of how their negative charge contributes to brain function. We have previously shown that intensely photoluminescent 9-nm diameter qua...

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Autores principales: Walters, Ryan, Medintz, Igor L., Delehanty, James B., Stewart, Michael H., Susumu, Kimihiro, Huston, Alan L., Dawson, Philip E., Dawson, Glyn
Formato: Online Artículo Texto
Lenguaje:English
Publicado: SAGE Publications 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4550297/
https://www.ncbi.nlm.nih.gov/pubmed/26243591
http://dx.doi.org/10.1177/1759091415592389
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author Walters, Ryan
Medintz, Igor L.
Delehanty, James B.
Stewart, Michael H.
Susumu, Kimihiro
Huston, Alan L.
Dawson, Philip E.
Dawson, Glyn
author_facet Walters, Ryan
Medintz, Igor L.
Delehanty, James B.
Stewart, Michael H.
Susumu, Kimihiro
Huston, Alan L.
Dawson, Philip E.
Dawson, Glyn
author_sort Walters, Ryan
collection PubMed
description Despite our extensive knowledge of the structure of negatively charged cell surface proteoglycans and sialoglycoconjugates in the brain, we have little understanding of how their negative charge contributes to brain function. We have previously shown that intensely photoluminescent 9-nm diameter quantum dots (QDs) with a CdSe core, a ZnS shell, and a negatively charged compact molecular ligand coating (CL4) selectively target neurons rather than glia. We now provide an explanation for this selective neuronal delivery. In this study, we compared three zwitterionic QD coatings differing only in their regions of positive or negative charge, as well as a positively charged (NH(2)) polyethylene glycol (PEG) coat, for their ability to deliver the cell-membrane-penetrating chaperone lipopeptide JB577 (WG(Palmitoyl)VKIKKP(9)G(2)H(6)) to individual cells in neonatal rat hippocampal slices. We confirm both that preferential uptake in neurons, and the lack of uptake in glia, is strongly associated with having a region of greater negative charge on the QD coating. In addition, the role of negatively charged chondroitin sulfate of the extracellular matrix (ECM) in restricting uptake was further suggested by digesting neonatal rat hippocampal slices with chondroitinase ABC and showing increased uptake of QDs by oligodendrocytes. Treatment still did not affect uptake in astrocytes or microglia. Finally, the future potential of using QDs as vehicles for trafficking proteins into cells continues to show promise, as we show that by administering a histidine-tagged green fluorescent protein (eGFP-His(6)) to hippocampal slices, we can observe neuronal uptake of GFP.
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spelling pubmed-45502972015-09-04 The Role of Negative Charge in the Delivery of Quantum Dots to Neurons Walters, Ryan Medintz, Igor L. Delehanty, James B. Stewart, Michael H. Susumu, Kimihiro Huston, Alan L. Dawson, Philip E. Dawson, Glyn ASN Neuro Original Article Despite our extensive knowledge of the structure of negatively charged cell surface proteoglycans and sialoglycoconjugates in the brain, we have little understanding of how their negative charge contributes to brain function. We have previously shown that intensely photoluminescent 9-nm diameter quantum dots (QDs) with a CdSe core, a ZnS shell, and a negatively charged compact molecular ligand coating (CL4) selectively target neurons rather than glia. We now provide an explanation for this selective neuronal delivery. In this study, we compared three zwitterionic QD coatings differing only in their regions of positive or negative charge, as well as a positively charged (NH(2)) polyethylene glycol (PEG) coat, for their ability to deliver the cell-membrane-penetrating chaperone lipopeptide JB577 (WG(Palmitoyl)VKIKKP(9)G(2)H(6)) to individual cells in neonatal rat hippocampal slices. We confirm both that preferential uptake in neurons, and the lack of uptake in glia, is strongly associated with having a region of greater negative charge on the QD coating. In addition, the role of negatively charged chondroitin sulfate of the extracellular matrix (ECM) in restricting uptake was further suggested by digesting neonatal rat hippocampal slices with chondroitinase ABC and showing increased uptake of QDs by oligodendrocytes. Treatment still did not affect uptake in astrocytes or microglia. Finally, the future potential of using QDs as vehicles for trafficking proteins into cells continues to show promise, as we show that by administering a histidine-tagged green fluorescent protein (eGFP-His(6)) to hippocampal slices, we can observe neuronal uptake of GFP. SAGE Publications 2015-07-20 /pmc/articles/PMC4550297/ /pubmed/26243591 http://dx.doi.org/10.1177/1759091415592389 Text en © The Author(s) 2015 http://creativecommons.org/licenses/by/3.0/ This article is distributed under the terms of the Creative Commons Attribution 3.0 License (http://www.creativecommons.org/licenses/by/3.0/) which permits any use, reproduction and distribution of the work without further permission provided the original work is attributed as specified on the SAGE and Open Access page (http://www.uk.sagepub.com/aboutus/openaccess.htm).
spellingShingle Original Article
Walters, Ryan
Medintz, Igor L.
Delehanty, James B.
Stewart, Michael H.
Susumu, Kimihiro
Huston, Alan L.
Dawson, Philip E.
Dawson, Glyn
The Role of Negative Charge in the Delivery of Quantum Dots to Neurons
title The Role of Negative Charge in the Delivery of Quantum Dots to Neurons
title_full The Role of Negative Charge in the Delivery of Quantum Dots to Neurons
title_fullStr The Role of Negative Charge in the Delivery of Quantum Dots to Neurons
title_full_unstemmed The Role of Negative Charge in the Delivery of Quantum Dots to Neurons
title_short The Role of Negative Charge in the Delivery of Quantum Dots to Neurons
title_sort role of negative charge in the delivery of quantum dots to neurons
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4550297/
https://www.ncbi.nlm.nih.gov/pubmed/26243591
http://dx.doi.org/10.1177/1759091415592389
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