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Physicochemical Properties and Route of Systemic Delivery Control the In Vivo Dynamics and Breakdown of Radiolabeled Gold Nanostars

The in vivo dynamics of nanoparticles requires a mechanistic understanding of multiple factors. Here, for the first time, the surprising breakdown of functionalized gold nanostars (F-AuNSs) conjugated with antibodies and (64)Cu radiolabels in vivo and in artificial lysosomal fluid ex vivo, is shown....

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Autores principales: Wen, Xiaona, Ou, Luping, Cutshaw, Gabriel, Uthaman, Saji, Ou, Yu-Chuan, Zhu, Tian, Szakas, Sarah, Carney, Brandon, Houghton, Jacob, Gundlach-Graham, Alexander, Rafat, Marjan, Yang, Kai, Bardhan, Rizia
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10518372/
https://www.ncbi.nlm.nih.gov/pubmed/36965074
http://dx.doi.org/10.1002/smll.202204293
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author Wen, Xiaona
Ou, Luping
Cutshaw, Gabriel
Uthaman, Saji
Ou, Yu-Chuan
Zhu, Tian
Szakas, Sarah
Carney, Brandon
Houghton, Jacob
Gundlach-Graham, Alexander
Rafat, Marjan
Yang, Kai
Bardhan, Rizia
author_facet Wen, Xiaona
Ou, Luping
Cutshaw, Gabriel
Uthaman, Saji
Ou, Yu-Chuan
Zhu, Tian
Szakas, Sarah
Carney, Brandon
Houghton, Jacob
Gundlach-Graham, Alexander
Rafat, Marjan
Yang, Kai
Bardhan, Rizia
author_sort Wen, Xiaona
collection PubMed
description The in vivo dynamics of nanoparticles requires a mechanistic understanding of multiple factors. Here, for the first time, the surprising breakdown of functionalized gold nanostars (F-AuNSs) conjugated with antibodies and (64)Cu radiolabels in vivo and in artificial lysosomal fluid ex vivo, is shown. The short-term biodistribution of F-AuNSs is driven by the route of systemic delivery (intravenous vs intraperitoneal) and long-term fate is controlled by the tissue type in vivo. In vitro studies including endocytosis pathways, intracellular trafficking, and opsonization, are combined with in vivo studies integrating a milieu of spectroscopy and microcopy techniques that show F-AuNSs dynamics is driven by their physicochemical properties and route of delivery. F-AuNSs break down into sub-20 nm broken nanoparticles as early as 7 days postinjection. Martini coarse-grained simulations are performed to support the in vivo findings. Simulations suggest that shape, size, and charge of the broken nanoparticles, and composition of the lipid membrane depicting various tissues govern the interaction of the nanoparticles with the membrane, and the rate of translocation across the membrane to ultimately enable tissue clearance. The fundamental study addresses critical gaps in the knowledge regarding the fate of nanoparticles in vivo that remain a bottleneck in their clinical translation.
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spelling pubmed-105183722023-09-28 Physicochemical Properties and Route of Systemic Delivery Control the In Vivo Dynamics and Breakdown of Radiolabeled Gold Nanostars Wen, Xiaona Ou, Luping Cutshaw, Gabriel Uthaman, Saji Ou, Yu-Chuan Zhu, Tian Szakas, Sarah Carney, Brandon Houghton, Jacob Gundlach-Graham, Alexander Rafat, Marjan Yang, Kai Bardhan, Rizia Small Article The in vivo dynamics of nanoparticles requires a mechanistic understanding of multiple factors. Here, for the first time, the surprising breakdown of functionalized gold nanostars (F-AuNSs) conjugated with antibodies and (64)Cu radiolabels in vivo and in artificial lysosomal fluid ex vivo, is shown. The short-term biodistribution of F-AuNSs is driven by the route of systemic delivery (intravenous vs intraperitoneal) and long-term fate is controlled by the tissue type in vivo. In vitro studies including endocytosis pathways, intracellular trafficking, and opsonization, are combined with in vivo studies integrating a milieu of spectroscopy and microcopy techniques that show F-AuNSs dynamics is driven by their physicochemical properties and route of delivery. F-AuNSs break down into sub-20 nm broken nanoparticles as early as 7 days postinjection. Martini coarse-grained simulations are performed to support the in vivo findings. Simulations suggest that shape, size, and charge of the broken nanoparticles, and composition of the lipid membrane depicting various tissues govern the interaction of the nanoparticles with the membrane, and the rate of translocation across the membrane to ultimately enable tissue clearance. The fundamental study addresses critical gaps in the knowledge regarding the fate of nanoparticles in vivo that remain a bottleneck in their clinical translation. 2023-07 2023-03-25 /pmc/articles/PMC10518372/ /pubmed/36965074 http://dx.doi.org/10.1002/smll.202204293 Text en https://creativecommons.org/licenses/by/4.0/This is an open access article under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Article
Wen, Xiaona
Ou, Luping
Cutshaw, Gabriel
Uthaman, Saji
Ou, Yu-Chuan
Zhu, Tian
Szakas, Sarah
Carney, Brandon
Houghton, Jacob
Gundlach-Graham, Alexander
Rafat, Marjan
Yang, Kai
Bardhan, Rizia
Physicochemical Properties and Route of Systemic Delivery Control the In Vivo Dynamics and Breakdown of Radiolabeled Gold Nanostars
title Physicochemical Properties and Route of Systemic Delivery Control the In Vivo Dynamics and Breakdown of Radiolabeled Gold Nanostars
title_full Physicochemical Properties and Route of Systemic Delivery Control the In Vivo Dynamics and Breakdown of Radiolabeled Gold Nanostars
title_fullStr Physicochemical Properties and Route of Systemic Delivery Control the In Vivo Dynamics and Breakdown of Radiolabeled Gold Nanostars
title_full_unstemmed Physicochemical Properties and Route of Systemic Delivery Control the In Vivo Dynamics and Breakdown of Radiolabeled Gold Nanostars
title_short Physicochemical Properties and Route of Systemic Delivery Control the In Vivo Dynamics and Breakdown of Radiolabeled Gold Nanostars
title_sort physicochemical properties and route of systemic delivery control the in vivo dynamics and breakdown of radiolabeled gold nanostars
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10518372/
https://www.ncbi.nlm.nih.gov/pubmed/36965074
http://dx.doi.org/10.1002/smll.202204293
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