Distribution and inflammatory cell response to intracranial delivery of radioluminescent Y2(SiO(4))O:Ce particles

Due to increasing advances in their manufacture and functionalization, nanoparticle-based systems have become a popular tool for in vivo drug delivery and biodetection. Recently, scintillating nanoparticles such as yttrium orthosilicate doped with cerium (Y2(SiO(4))O:Ce) have come under study for th...

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Autores principales: Fischer, Máté, Zimmerman, Amber, Zhang, Eric, Kolis, Joseph, Dickey, Ashley, Burdette, Mary K., Chander, Praveen, Foulger, Stephen H., Brigman, Jonathan L., Weick, Jason P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9836305/
https://www.ncbi.nlm.nih.gov/pubmed/36634053
http://dx.doi.org/10.1371/journal.pone.0276819
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author Fischer, Máté
Zimmerman, Amber
Zhang, Eric
Kolis, Joseph
Dickey, Ashley
Burdette, Mary K.
Chander, Praveen
Foulger, Stephen H.
Brigman, Jonathan L.
Weick, Jason P.
author_facet Fischer, Máté
Zimmerman, Amber
Zhang, Eric
Kolis, Joseph
Dickey, Ashley
Burdette, Mary K.
Chander, Praveen
Foulger, Stephen H.
Brigman, Jonathan L.
Weick, Jason P.
author_sort Fischer, Máté
collection PubMed
description Due to increasing advances in their manufacture and functionalization, nanoparticle-based systems have become a popular tool for in vivo drug delivery and biodetection. Recently, scintillating nanoparticles such as yttrium orthosilicate doped with cerium (Y2(SiO(4))O:Ce) have come under study for their potential utility in optogenetic applications, as they emit photons upon low levels of stimulation from remote x-ray sources. The utility of such nanoparticles in vivo is hampered by rapid clearance from circulation by the mononuclear phagocytic system, which heavily restricts nanoparticle accumulation at target tissues. Local transcranial injection of nanoparticles may deliver scintillating nanoparticles to highly specific brain regions by circumventing the blood-brain barrier and avoiding phagocytic clearance. Few studies to date have examined the distribution and response to nanoparticles following localized delivery to cerebral cortex, a crucial step in understanding the therapeutic potential of nanoparticle-based biodetection in the brain. Following the synthesis and surface modification of these nanoparticles, two doses (1 and 3 mg/ml) were introduced into mouse secondary motor cortex (M2). This region was chosen as the site for RLP delivery, as it represents a common target for optogenetic manipulations of mouse behavior, and RLPs could eventually serve as an injectable x-ray inducible light delivery system. The spread of particles through the target tissue was assessed 24 hours, 72 hours, and 9 days post-injection. Y2(SiO(4))O:Ce nanoparticles were found to be detectable in the brain for up to 9 days, initially diffusing through the tissue until 72 hours before achieving partial clearance by the final endpoint. Small transient increases in the presence of IBA-1(+) microglia and GFAP(+) astrocytic cell populations were detected near nanoparticle injection sites of both doses tested 24 hours after surgery. Taken together, these data provide evidence that Y2(SiO(4))O:Ce nanoparticles coated with BSA can be injected directly into mouse cortex in vivo, where they persist for days and are broadly tolerated, such that they may be potentially utilized for remote x-ray activated stimulation and photon emission for optogenetic experiments in the near future.
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spelling pubmed-98363052023-01-13 Distribution and inflammatory cell response to intracranial delivery of radioluminescent Y2(SiO(4))O:Ce particles Fischer, Máté Zimmerman, Amber Zhang, Eric Kolis, Joseph Dickey, Ashley Burdette, Mary K. Chander, Praveen Foulger, Stephen H. Brigman, Jonathan L. Weick, Jason P. PLoS One Research Article Due to increasing advances in their manufacture and functionalization, nanoparticle-based systems have become a popular tool for in vivo drug delivery and biodetection. Recently, scintillating nanoparticles such as yttrium orthosilicate doped with cerium (Y2(SiO(4))O:Ce) have come under study for their potential utility in optogenetic applications, as they emit photons upon low levels of stimulation from remote x-ray sources. The utility of such nanoparticles in vivo is hampered by rapid clearance from circulation by the mononuclear phagocytic system, which heavily restricts nanoparticle accumulation at target tissues. Local transcranial injection of nanoparticles may deliver scintillating nanoparticles to highly specific brain regions by circumventing the blood-brain barrier and avoiding phagocytic clearance. Few studies to date have examined the distribution and response to nanoparticles following localized delivery to cerebral cortex, a crucial step in understanding the therapeutic potential of nanoparticle-based biodetection in the brain. Following the synthesis and surface modification of these nanoparticles, two doses (1 and 3 mg/ml) were introduced into mouse secondary motor cortex (M2). This region was chosen as the site for RLP delivery, as it represents a common target for optogenetic manipulations of mouse behavior, and RLPs could eventually serve as an injectable x-ray inducible light delivery system. The spread of particles through the target tissue was assessed 24 hours, 72 hours, and 9 days post-injection. Y2(SiO(4))O:Ce nanoparticles were found to be detectable in the brain for up to 9 days, initially diffusing through the tissue until 72 hours before achieving partial clearance by the final endpoint. Small transient increases in the presence of IBA-1(+) microglia and GFAP(+) astrocytic cell populations were detected near nanoparticle injection sites of both doses tested 24 hours after surgery. Taken together, these data provide evidence that Y2(SiO(4))O:Ce nanoparticles coated with BSA can be injected directly into mouse cortex in vivo, where they persist for days and are broadly tolerated, such that they may be potentially utilized for remote x-ray activated stimulation and photon emission for optogenetic experiments in the near future. Public Library of Science 2023-01-12 /pmc/articles/PMC9836305/ /pubmed/36634053 http://dx.doi.org/10.1371/journal.pone.0276819 Text en © 2023 Fischer et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Fischer, Máté
Zimmerman, Amber
Zhang, Eric
Kolis, Joseph
Dickey, Ashley
Burdette, Mary K.
Chander, Praveen
Foulger, Stephen H.
Brigman, Jonathan L.
Weick, Jason P.
Distribution and inflammatory cell response to intracranial delivery of radioluminescent Y2(SiO(4))O:Ce particles
title Distribution and inflammatory cell response to intracranial delivery of radioluminescent Y2(SiO(4))O:Ce particles
title_full Distribution and inflammatory cell response to intracranial delivery of radioluminescent Y2(SiO(4))O:Ce particles
title_fullStr Distribution and inflammatory cell response to intracranial delivery of radioluminescent Y2(SiO(4))O:Ce particles
title_full_unstemmed Distribution and inflammatory cell response to intracranial delivery of radioluminescent Y2(SiO(4))O:Ce particles
title_short Distribution and inflammatory cell response to intracranial delivery of radioluminescent Y2(SiO(4))O:Ce particles
title_sort distribution and inflammatory cell response to intracranial delivery of radioluminescent y2(sio(4))o:ce particles
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9836305/
https://www.ncbi.nlm.nih.gov/pubmed/36634053
http://dx.doi.org/10.1371/journal.pone.0276819
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