Cell–Surface Binding of DNA Nanostructures for Enhanced Intracellular and Intranuclear Delivery
Weitao Wang
1
,
Bhavya Chopra
2
,
Vismaya Walawalkar
1
,
Zijuan Liang
1
,
Rebekah Adams
1
,
Markus Deserno
3
,
Xi Ren
1, 2
,
Rebecca Taylor
1, 2, 4
3
Publication type: Journal Article
Publication date: 2024-03-18
scimago Q1
wos Q1
SJR: 1.921
CiteScore: 14.5
Impact factor: 8.2
ISSN: 19448244, 19448252
PubMed ID:
38497300
General Materials Science
Abstract
DNA nanostructures (DNs) have found increasing use in biosensing, drug delivery, and therapeutics because of their customizable assembly, size and shape control, and facile functionalization. However, their limited cellular uptake and nuclear delivery have hindered their effectiveness in these applications. Here, we demonstrate the potential of applying cell-surface binding as a general strategy to enable rapid enhancement of intracellular and intranuclear delivery of DNs. By targeting the plasma membrane via cholesterol anchors or the cell-surface glycocalyx using click chemistry, we observe a significant 2 to 8-fold increase in the cellular uptake of three distinct types of DNs that include nanospheres, nanorods, and nanotiles, within a short time frame of half an hour. Several factors are found to play a critical role in modulating the uptake of DNs, including their geometries, the valency, positioning and spacing of binding moieties. Briefly, nanospheres are universally preferable for cell surface attachment and internalization. However, edge-decorated nanotiles compensate for their geometry deficiency and outperform nanospheres in both categories. In addition, we confirm the short-term structural stability of DNs by incubating them with cell medium and cell lysate. Further, we investigate the endocytic pathway of cell-surface bound DNs and reveal that it is an interdependent process involving multiple pathways, similar to those of unmodified DNs. Finally, we demonstrate that cell-surface attached DNs exhibit a substantial enhancement in the intranuclear delivery. Our findings present an application that leverages cell-surface binding to potentially overcome the limitations of low cellular uptake, which may strengthen and expand the toolbox for effective cellular and nuclear delivery of DNA nanostructure systems.
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Metrics
7
Total citations:
7
Citations from 2024:
7
(100%)
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GOST
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Wang W. et al. Cell–Surface Binding of DNA Nanostructures for Enhanced Intracellular and Intranuclear Delivery // ACS applied materials & interfaces. 2024. Vol. 16. No. 13. pp. 15783-15797.
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Wang W., Chopra B., Walawalkar V., Liang Z., Adams R., Deserno M., Ren X., Taylor R. Cell–Surface Binding of DNA Nanostructures for Enhanced Intracellular and Intranuclear Delivery // ACS applied materials & interfaces. 2024. Vol. 16. No. 13. pp. 15783-15797.
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RIS
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TY - JOUR
DO - 10.1021/acsami.3c18068
UR - https://pubs.acs.org/doi/10.1021/acsami.3c18068
TI - Cell–Surface Binding of DNA Nanostructures for Enhanced Intracellular and Intranuclear Delivery
T2 - ACS applied materials & interfaces
AU - Wang, Weitao
AU - Chopra, Bhavya
AU - Walawalkar, Vismaya
AU - Liang, Zijuan
AU - Adams, Rebekah
AU - Deserno, Markus
AU - Ren, Xi
AU - Taylor, Rebecca
PY - 2024
DA - 2024/03/18
PB - American Chemical Society (ACS)
SP - 15783-15797
IS - 13
VL - 16
PMID - 38497300
SN - 1944-8244
SN - 1944-8252
ER -
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BibTex (up to 50 authors)
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@article{2024_Wang,
author = {Weitao Wang and Bhavya Chopra and Vismaya Walawalkar and Zijuan Liang and Rebekah Adams and Markus Deserno and Xi Ren and Rebecca Taylor},
title = {Cell–Surface Binding of DNA Nanostructures for Enhanced Intracellular and Intranuclear Delivery},
journal = {ACS applied materials & interfaces},
year = {2024},
volume = {16},
publisher = {American Chemical Society (ACS)},
month = {mar},
url = {https://pubs.acs.org/doi/10.1021/acsami.3c18068},
number = {13},
pages = {15783--15797},
doi = {10.1021/acsami.3c18068}
}
Cite this
MLA
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Wang, Weitao, et al. “Cell–Surface Binding of DNA Nanostructures for Enhanced Intracellular and Intranuclear Delivery.” ACS applied materials & interfaces, vol. 16, no. 13, Mar. 2024, pp. 15783-15797. https://pubs.acs.org/doi/10.1021/acsami.3c18068.