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Neutrophil as a Carrier for Cancer Nanotherapeutics: A Comparative Study of Liposome, PLGA, and Magnetic Nanoparticles Delivery to Tumors

Insufficient drug accumulation in tumors is still a major concern for using cancer nanotherapeutics. Here, the neutrophil-based delivery of three nanoparticle types—liposomes, PLGA, and magnetite nanoparticles—was assessed both in vitro and in vivo. Confocal microscopy and a flow cytometry analysis...

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Autores principales: Garanina, Anastasiia S., Vishnevskiy, Daniil A., Chernysheva, Anastasia A., Valikhov, Marat P., Malinovskaya, Julia A., Lazareva, Polina A., Semkina, Alevtina S., Abakumov, Maxim A., Naumenko, Victor A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10674452/
https://www.ncbi.nlm.nih.gov/pubmed/38004431
http://dx.doi.org/10.3390/ph16111564
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author Garanina, Anastasiia S.
Vishnevskiy, Daniil A.
Chernysheva, Anastasia A.
Valikhov, Marat P.
Malinovskaya, Julia A.
Lazareva, Polina A.
Semkina, Alevtina S.
Abakumov, Maxim A.
Naumenko, Victor A.
author_facet Garanina, Anastasiia S.
Vishnevskiy, Daniil A.
Chernysheva, Anastasia A.
Valikhov, Marat P.
Malinovskaya, Julia A.
Lazareva, Polina A.
Semkina, Alevtina S.
Abakumov, Maxim A.
Naumenko, Victor A.
author_sort Garanina, Anastasiia S.
collection PubMed
description Insufficient drug accumulation in tumors is still a major concern for using cancer nanotherapeutics. Here, the neutrophil-based delivery of three nanoparticle types—liposomes, PLGA, and magnetite nanoparticles—was assessed both in vitro and in vivo. Confocal microscopy and a flow cytometry analysis demonstrated that all the studied nanoparticles interacted with neutrophils from the peripheral blood of mice with 4T1 mammary adenocarcinoma without a significant impact on neutrophil viability or activation state. Intravital microscopy of the tumor microenvironment showed that the neutrophils did not engulf the liposomes after intravenous administration, but facilitated nanoparticle extravasation in tumors through micro- and macroleakages. PLGA accumulated along the vessel walls in the form of local clusters. Later, PLGA nanoparticle-loaded neutrophils were found to cross the vascular barrier and migrate towards the tumor core. The magnetite nanoparticles extravasated in tumors both via spontaneous macroleakages and on neutrophils. Overall, the specific type of nanoparticles largely determined their behavior in blood vessels and their neutrophil-mediated delivery to the tumor. Since neutrophils are the first to migrate to the site of inflammation, they can increase nanodrug delivery effectiveness for nanomedicine application.
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spelling pubmed-106744522023-11-06 Neutrophil as a Carrier for Cancer Nanotherapeutics: A Comparative Study of Liposome, PLGA, and Magnetic Nanoparticles Delivery to Tumors Garanina, Anastasiia S. Vishnevskiy, Daniil A. Chernysheva, Anastasia A. Valikhov, Marat P. Malinovskaya, Julia A. Lazareva, Polina A. Semkina, Alevtina S. Abakumov, Maxim A. Naumenko, Victor A. Pharmaceuticals (Basel) Article Insufficient drug accumulation in tumors is still a major concern for using cancer nanotherapeutics. Here, the neutrophil-based delivery of three nanoparticle types—liposomes, PLGA, and magnetite nanoparticles—was assessed both in vitro and in vivo. Confocal microscopy and a flow cytometry analysis demonstrated that all the studied nanoparticles interacted with neutrophils from the peripheral blood of mice with 4T1 mammary adenocarcinoma without a significant impact on neutrophil viability or activation state. Intravital microscopy of the tumor microenvironment showed that the neutrophils did not engulf the liposomes after intravenous administration, but facilitated nanoparticle extravasation in tumors through micro- and macroleakages. PLGA accumulated along the vessel walls in the form of local clusters. Later, PLGA nanoparticle-loaded neutrophils were found to cross the vascular barrier and migrate towards the tumor core. The magnetite nanoparticles extravasated in tumors both via spontaneous macroleakages and on neutrophils. Overall, the specific type of nanoparticles largely determined their behavior in blood vessels and their neutrophil-mediated delivery to the tumor. Since neutrophils are the first to migrate to the site of inflammation, they can increase nanodrug delivery effectiveness for nanomedicine application. MDPI 2023-11-06 /pmc/articles/PMC10674452/ /pubmed/38004431 http://dx.doi.org/10.3390/ph16111564 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Garanina, Anastasiia S.
Vishnevskiy, Daniil A.
Chernysheva, Anastasia A.
Valikhov, Marat P.
Malinovskaya, Julia A.
Lazareva, Polina A.
Semkina, Alevtina S.
Abakumov, Maxim A.
Naumenko, Victor A.
Neutrophil as a Carrier for Cancer Nanotherapeutics: A Comparative Study of Liposome, PLGA, and Magnetic Nanoparticles Delivery to Tumors
title Neutrophil as a Carrier for Cancer Nanotherapeutics: A Comparative Study of Liposome, PLGA, and Magnetic Nanoparticles Delivery to Tumors
title_full Neutrophil as a Carrier for Cancer Nanotherapeutics: A Comparative Study of Liposome, PLGA, and Magnetic Nanoparticles Delivery to Tumors
title_fullStr Neutrophil as a Carrier for Cancer Nanotherapeutics: A Comparative Study of Liposome, PLGA, and Magnetic Nanoparticles Delivery to Tumors
title_full_unstemmed Neutrophil as a Carrier for Cancer Nanotherapeutics: A Comparative Study of Liposome, PLGA, and Magnetic Nanoparticles Delivery to Tumors
title_short Neutrophil as a Carrier for Cancer Nanotherapeutics: A Comparative Study of Liposome, PLGA, and Magnetic Nanoparticles Delivery to Tumors
title_sort neutrophil as a carrier for cancer nanotherapeutics: a comparative study of liposome, plga, and magnetic nanoparticles delivery to tumors
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10674452/
https://www.ncbi.nlm.nih.gov/pubmed/38004431
http://dx.doi.org/10.3390/ph16111564
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